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Generate impression based on findings.
Reason: cognitive impairment - h/o breast CA History: cognitive decline, behavioral changes The CSF spaces are appropriate for the patient's stated age with no midline shift. There is a moderate degree of periventricular and subcortical punctate hyperintense white matter lesions present identified on the FLAIR and T2 images. There also punctate lesions present in the brainstem which are high signal on T2 and flair MRI.No abnormal enhancing mass lesions are appreciated intracranially. No intracranial hemorrhage is identified. No edema is identified within the brain parenchyma.Normal vascular flow voids are present in the distal carotid and vertebral arteries, the basilar artery and the proximal anterior, middle and posterior cerebral arteries as well as the internal cerebral veins and superior sagittal sinus.The visualized portions of the paranasal sinuses are clear. The visualized portions of the mastoid air cells are clear. The visualized portions of the orbits are intact. The right eyeball lens is thin.
1.Periventricular and subcortical white matter changes of a moderate degree and a small lesion in the brainstem are nonspecific. At this age they are most likely vascular related. 2.No abnormal enhancing lesions are identified intracranially to suggest brain metastases
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57-year-old male, evaluate right total rotator cuff ROTATOR CUFF: There is a full-thickness tear of the distal supraspinatus tendon with approximately 1 cm retraction. Extensive increased T2 signal in the distal supraspinous infraspinous tendons indicate associated tendinosis. The teres minor and subscapularis are intact. There is no significant muscular atrophy.SUPRASPINATUS OUTLET: Moderate acromioclavicular joint osteoarthritis. Fluid extends within the subdeltoid bursa.GLENOHUMERAL JOINT AND GLENOID LABRUM: There is globular increased signal within the superior labrum, likely representing degeneration.BICEPS TENDON: The long head of biceps tendon is normally situated within the bicipital groove.ADDITIONAL
1. Full thickness rotator cuff tear with retraction as described above.2. Acromioclavicular and glenohumeral degenerative changes as described above.
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Lumbar spine CT for planning pedicle screw fusion at L4-L5. There is grade 1 anterolisthesis of L4. Vertebral body heights are maintained. Multilevel anterior osteophytes are consistent with osteoarthritis. The caliber of the lumbar spinal canal appears small.At L1/L2, L2/L3, and L3/L4, there is mild diffuse disk bulge and disk space narrowing without significant compromise to the spinal canal or neural foramina. Schmorl's nodes are again identified at the superior endplate of L2 and inferior endplate of L3.At L4/L5 there is grade 1 anterolisthesis of L4. In addition, there is a diffuse disk bulge, subchondral sclerosis, bilateral facet and ligamentum flavum hypertrophy causing moderate to marked central spinal stenosis and bilateral encroachment of the lateral recesses, right greater than left. Neural foraminal narrowing is identified on the right. Synovial cyst identified at this level on the prior MRI is not identified on today's CT.At L5/S1, there is diffuse disk bulge and loss of disk space height without compromise to the central spinal canal or neural foramina.
Degenerative changes most prominent at L4-L5 consisting of a diffuse disk bulge, hypertrophic facet and ligamentum flavum changes, and mild anterolisthesis causing central spinal stenosis, encroachment of bilateral lateral recesses, right greater than left, and neural foramina narrowing on the right. The patient had a synovial cyst demonstrated on the prior exam at L4-5. This exam is not sensitive to detecting synovial cyst.
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59-year-old male with history of right renal mass. ABDOMEN:LIVER, BILIARY TRACT: Multiple enhancing liver lesions likely representing metastatic disease. For reference, a segment 7 lesion measures 1.7 x 1.1 cm (image 7 of series 10).SPLEEN: No significant abnormality noted.PANCREAS: No significant abnormality noted.ADRENAL GLANDS: No significant abnormality noted.KIDNEYS, URETERS: Left inferior pole solid lesion with peripheral enhancement and central necrosis measures 9.3 x 9.1 cm (image 66 of series 10). This lesion is compatible with RCC. There is a persistent, nonenhancing filling defect extending from the right renal vein into the infrahepatic IVC approaching the intrahepatic segment.The left kidney is unremarkable.RETROPERITONEUM, LYMPH NODES: No significant abnormality noted.BOWEL, MESENTERY: No significant abnormality noted.BONES, SOFT TISSUES: No significant abnormality noted.OTHER: There are multiple nodules located within the right lower lobe likely representing metastatic disease.
1. Large left inferior pole renal mass compatible with RCC. Persistent filling defect extending from the right renal vein to the infrahepatic IVC compatible with bland thrombus.2. Multiple enhancing hepatic lesions, nonspecific, but likely compatible with metastatic disease.3. Partially imaged pulmonary nodules compatible with metastatic disease. CT chest recommended for further evaluation.
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End-stage renal disease on hemodialysis with left toe stump infection. Evaluate for osteomyelitis. TENDONS: No significant abnormality noted.LIGAMENTS: No significant abnormality noted.ARTICULAR SURFACES AND BONE: Patient is status post amputation of the first toe through the base of the proximal phalanx. There is no bone marrow edema to suggest osteomyelitis. ADDITIONAL
Lobulated collection about the distal first metatarsal stump, may represent an abscess. No bone marrow abnormality to suggest osteomyelitis.
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The cerebellar tonsils are in appropriate position, without ectopia, demonstrating a normal rounded morphology. Sagittal CSF flow demonstrates biphasic flow anteriorly and posteriorly at the level of the foramen magnum and cerebellar tonsils.Brain MRI:The ventricles and sulci are normal in size. There are no masses, mass effect or midline shift. The pituitary gland is normal in size. There is no evidence for intracranial hemorrhage or acute cerebral, brainstem or cerebellar infarction. No diffusion-weighted abnormalities are identified. There are no extraaxial fluid collections or subdural hematomas. Flow voids are present within the major vessels indicating patency. The paranasal sinuses and mastoid air cells are clear. Complete spine MRI:Alignment is anatomic. There are no fractures or subluxations. There are no osseous dysplasias. The marrow signal is benign. The cord and conus are normal in signal characteristics and caliber throughout. The conus terminates at L1/2. The visualized intra-abdominal and paraspinal contents are unremarkable. No fat signal abnormality is noted within the filum terminale.
1.The cerebellar tonsils are in appropriate position, without ectopia, demonstrating a normal rounded morphology.2.Negative noncontrast MRI of the brain and complete spine.
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Male, 79 years old, with left lower back pain. Evaluate for lumbar spine/sacroiliac disease. A moderate compression deformity of the T12 vertebral body with evidence of prior kyphoplasty is redemonstrated without significant interval change. The remaining vertebral bodies demonstrate preservation of height. Straightening of the cervical lordosis is seen. Endplate degenerative marrow signal is seen at L4-5, worse than on the prior examination, and to a lesser degree at L3-4, improved from prior.The visualized distal spinal cord, conus and cauda equina are within normal limits. No epidural abnormalities are suspected.L1-2: Loss of disc T2 signal but relative preservation of disc height. No significant spinal canal or foraminal stenosis. L2-3: Facet arthropathy and ligamentum flavum thickening. Loss of disc T2 signal but relative preservation of disc height. Mild predominantly lateral disc bulging. No significant generalized spinal canal stenosis. Mild bilateral foraminal narrowing. Findings have slightly progressed from prior. L3-4: Facet arthropathy and ligamentum flavum thickening. Mild loss of disc height and disc bulging. A previously seen left paracentral/foraminal protrusion is less conspicuous, but bilateral lateral bulging results in effacement of both lateral recesses and moderately severe narrowing of the neural foramina. These findings have progressed from prior. There is also a moderate generalized spinal canal narrowing. L4-5: Facet arthropathy and ligamentum flavum thickening. Bulging disc. Moderate to severe spinal canal narrowing with crowding of the cauda equina. Severe left foraminal narrowing with likely nerve impingement. Moderate to severe right foraminal narrowing. Findings have progressed from prior. L5-S1: Facet arthropathy and ligamentum flavum thickening. Bulging disc with a right paracentral protrusion. No significant generalized spinal canal stenosis. Severe right and moderate to severe left foraminal narrowing. Findings have progressed from prior. Sclerosis and osteophyte formation at the sacroiliac joints is partially visualized on this examination.
Disc and posterior element degeneration has progressed at multiple levels. At L3-4, this results in moderate generalized spinal canal stenosis and moderate left foraminal narrowing. At L4-5, this results in a moderate to severe spinal canal stenosis, severe left and moderate to severe right foraminal narrowing.
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47-year-old male with right knee pain. Evaluate for meniscal tear. MENISCI: There is globular increased signal intensity within the anterior horn of the lateral meniscus that appears to extend to the tibial articular surface suggestive of a degenerative undersurface tear. There is edema type signal abnormality within the soft tissues anterior to the lateral meniscus which may represent extension of mucoid material from the anterior horn. There is globular signal intensity within the posterior horn of the medial meniscus which likely represents mucoid degeneration, but we see no discrete tear.ARTICULAR CARTILAGE AND BONE: There appears to be diffuse articular cartilage loss along the medial facet of the patella. The articular cartilage otherwise appears normal for age. The bone marrow signal intensity is within normal limits. There is a broad-based bony excrescence extending from the medial aspect of the proximal fibula which may represent a 'tug lesion' at the soleus muscle origin, of doubtful significance. LIGAMENTS: There is mild increased signal intensity within the proximal fibers of the lateral collateral ligament proper which may reflect degeneration. There is also mild intermediate signal intensity between the IT band and lateral femoral condyle which may reflect mild inflammation. The cruciate ligaments appear intact.EXTENSOR MECHANISM: The extensor mechanism appears intact.ADDITIONAL
1. Findings suggestive of a degenerative tear of the anterior horn of the lateral meniscus.2. Edema and fluid tracking along the medial aspect of the gastrocnemius may represent a ruptured Baker's cyst.3. Other findings as described above.
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56 year old female with history of myocardial bridging, pericardial cyst and aortic regurgitation presenting for evaluation of chest painMEDICATIONS: aspirin First Pass PerfusionDuring hyperemia, no perfusion defects were present. There is dark rim artifact seen. Viability/ Myocardial ScarThere was no late gadolinium enhancement noted suggesting that there is no prior myocardial infarction, fibrosis, inflammation, or infiltration. The entire myocardium is viable. Left VentricleThe left ventricle is normal in size and systolic function. The overall LV ejection fraction is 55%, the LV end diastolic volume index is 78 ml/m2 (normal range: 65+/-11), the LVEDV is 147 ml (normal range 109+/-23), the LV end systolic volume index is 35 ml/m2 (normal range 18+/-5), the LVESV is 66 ml (normal range 31+/-10), the LV mass index is 22 g/m2, and the LV mass is 42 g. There are no regional wall motion abnormalities present. Left AtriumThe left atrium is normal in size. Right VentricleThe right ventricle is normal in size and systolic function. The overall RV ejection fraction is 54%, the RV end diastolic volume index is 85 ml/m2 (normal range 69+/-14), the RVEDV is 160 ml (normal range 110+/-24), the RV end systolic volume index is 39 ml/m2 (normal range 22+/-8), and the RVESV is 74 ml (normal range 35+/-13). Right AtriumThe right atrium is normal in size and function. Aortic ValveThe aortic valve opens widely and there is at least mild regurgitation. The regurgitant fraction is 13%. Mitral ValveThe mitral valve opens widely and there is no significant mitral regurgitation.Pulmonic ValveThe pulmonic valve opens widely. There is no significant pulmonic regurgitation.Tricuspid ValveThe tricuspid valve opens widely. There is no significant tricuspid regurgitation.AortaThe aortic root is normal in size (SoV 32 mm, ascending aorta 24mm). There is a left sided aortic arch with a normal brachiocephalic branching pattern.Pulmonary VeinsAll four pulmonary veins drain normally into the left atrium.Pulmonary ArteryThe main pulmonary artery is normal in size. Venous AnatomyThe SVC and IVC are drains normally into the right atrium. PericardiumThere is no obvious pericardial disease.Extracardiac FindingsThis study is not designed for the specific evaluation of extra-cardiac findings; therefore, the differentiation between artifacts and real extracardiac pathology may be difficult. If clinically indicated, a separate dedicated evaluation should be considered.
1. No perfusion defects/ "ischemia" present during hyperemia.2. No prior myocardial infarction. The entire myocardium is viable.3. Normal LV size and systolic function (LVEF 55%).4. Normal RV size and systolic function (RVEF 54%).I personally reviewed the Images and/or procedure with the Resident/Fellow and agree with this report.
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86-year-old female with altered mental status and history of transient ischemic attack x 2. Rule out ischemia. There is no evidence of intracranial hemorrhage, mass or edema. Small lacunae in the right basal ganglia. Few diffuse hypodensities consistent with minimal small vessel disease, age indeterminate, essentially within normal limits for the patient's age. If there is clinical concern for acute ischemia an MRI may be considered.The ventricles and basal cisterns are normal in size and configuration.The calvaria and skull base are radiographically normal. The visualized paranasal sinuses and mastoid air cells are normally pneumatized.
Minimal small vessel disease, age indeterminate. If there is clinical concern for acute ischemia an MRI may be considered.
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Lateral knee pain. Evaluate meniscus. MENISCI: There is a radial tear of the body of the lateral meniscus with a horizontal component. There is an adjacent increased T2 signal collection compatible with parameniscal cyst formation. The medial meniscus is intact. ARTICULAR CARTILAGE AND BONE: Bone marrow signal is within normal limits. The articular cartilage within all three compartments is intact.LIGAMENTS: The cruciate ligaments, collateral ligaments, and popliteus muscle/tendon are intact.EXTENSOR MECHANISM: No significant abnormality noted.ADDITIONAL
Complex tear of the body of the lateral meniscus with radial and horizontal components.
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50 years Male (DOB:8/19/1966)Reason: lumbar DDD History: back painPROVIDER/ATTENDING NAME: TARIQ MUSLIM MALIK SERVICES ANCILLARY Five lumbar type vertebral bodies are presumed to be present which are appropriate in overall alignment and height. The conus medullaris on sagittal imaging is grossly intact. There is accumulation of epidural fat within the lower lumbar spine especially below the L3 level associated with crowding of nerve roots in the sacral spinal canal and to a lesser degree elsewhere.At L5-S1 there is disc desiccation and diffuse disc bulge associated with marked bilateral facet hypertrophy and encroachment of the nerve roots of the left neural foramen.At L4-5 there is no significant compromise to spinal canal or neural foramina.At L3-4 there is no significant compromise to spinal canal or neural foramina.At L2-3 there is no significant compromise to spinal canal or neural foramina.At L1-2 there is no significant compromise to spinal canal or neural foramina.
1.Epidural lipomatosis is associated with stenosis in the lower lumbar spine especially the sacral spinal canal.2.There are degenerative changes present in the lumbar spine worse at L5-S1 there is marked facet hypertrophy in the chronic treatment of exiting nerve roots within the left neural foramen.
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Clinical question: Assess for epidural hematoma after epidural steroid injection last week. Signs and symptoms: Subjective right leg weakness and increased urinary frequency. Pre- and post enhanced lumbar MRI:Examination demonstrates a posterior epidural collection with mixed T2 and T1 signal intensity along the dorsal aspect of the spinal canal at L4-L5 disc level. It measures approximately 25 mm in cranial cephalad axis and 7 x 12 mm in transaxial dimensions. Finding is highly suspected of a small epidural hemorrhage. It results in subtle mass effect on the thecal sac posteriorly. On prior MRI exam from 3-20 2-15 from St. Alexius Medical Center there is also a central disc protrusion at this level with mass effect on the thecal sac which in combination with the epidural collection results in significant central spinal stenosis at this level. There is no significant neural foraminal compromise.Advanced degenerative disc disease at L4-L5 and moderate bilateral facet and ligamentum flavum hypertrophy is also noted at this level.Examination at L3-L4 demonstrate moderate disc disease, broad base bulging disc and moderate hypertrophic changes of posterior elements with resultant significant central spinal stenosis. There is no significant change of this finding since prior outside institution lumbar MRI. A tiny central disc extrusion at this level is also noted.Moderate disc disease and hypertrophic changes of posterior elements at L5-S1 as well as a small left paramedian disc protrusion without central spinal stenosis or significant neural foraminal compromise is noted. Mild degenerative changes at other levels however without central spinal stenosis.
1.At L4-L5 there is a small posterior epidural hemorrhage which in combination with a large central disc protrusion results in significant central spinal stenosis.2.At L3-L4 extensive degenerative changes also results in significant central spinal stenosis. No change since prior outside institute exam.3.At L5-S1 degenerative changes and including a left paramedian disc protrusion without spinal stenosis is present.
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Female, 72 years old, with adenocarcinoma of the lung and brain metastases, on chemotherapy. Image quality is somewhat reduced relative to the prior examination which reduces sensitivity for lesional changes.Linear enhancement without edema in the right superior parietal lobule may be slightly smaller than on the prior examination, now measuring up to 8 mm, previously 10 mm. A right cerebellar enhancing lesion without edema measures up to 7 mm, previously 7 mm. Three or four small foci of enhancement within the left perirolandic white matter are not as well seen on the present examination which could simply reflect differences in image quality.An enhancing nodule within the left middle frontal gyrus is less well-defined than on the prior examination and difficult to measure accurately. However, the degree of edema associated with this lesion has decreased.No convincing evidence of any new enhancing lesion is seen. Scattered foci of nonenhancing, nonspecific white matter T2 hyperintensity are seen, some of which may be new from prior. No significant mass effect is detected. The ventricular system is stable and within normal limits.
1.No definite evidence of any progression in the numerous previously described enhancing lesions.2.No convincing evidence of any new intracranial lesion is seen. However, the image quality on this examination is somewhat less than on the prior exam, which reduces the accuracy of comparison and the sensitivity for new lesion detection.
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16 year old male with history of recent myocarditis and clinical VT, with recurrent arrhythmias now referred for repeat cardiac MR to evaluate scar burden and function. Left VentricleThe left ventricle is normal in size with normal systolic function. The overall LV ejection fraction is 61%, the LV end diastolic volume index is 73 ml/m2 (normal range: 74+/-15), the LVEDV is 146 ml (normal range 142+/-34), the LV end systolic volume index is 29 ml/m2 (normal range 25+/-9), the LVESV is 57 ml (normal range 47+/-19), the LV mass index is 43 g/m2 (normal range 85+/-15), and the LV mass is 87 g (normal range 164+/-36). There are no regional wall motion abnormalities present. There is persistence of epicardial late gadolinium enhancement in the basal anterolateral and small segment of the mid inferolateral walls, but overall there is less myocardial involvement on this study. This pattern of late gadolinium enhancement is typical for prior myocarditis. The T2-STIR signal in the inferolateral and lateral walls seen on the previous study suggesting myocardial edema are no longer present; additionally the global relative enhancement ratio is normal.Left AtriumThe left atrium is normal in size. Right VentricleThe right ventricle is normal in size with normal systolic function. The overall RV ejection fraction is 50%, the RV end diastolic volume index is 79 ml/m2 (normal range 82+/-16), the RVEDV is 158 ml (normal range 142+/-31), the RV end systolic volume index is 40 ml/m2 (normal range 31+/-9), and the RVESV is 80 ml (normal range 54+/-17).Right AtriumThe right atrium is normal in size.Aortic ValveThe aortic valve opens widely and there is no significant aortic regurgitation.Mitral ValveThe mitral valve opens widely and there is no significant mitral regurgitation.Pulmonic ValveThe pulmonic valve opens widely. There is no significant pulmonic regurgitation.Tricuspid ValveThe tricuspid valve opens widely. There is no significant tricuspid regurgitation.AortaThere is a left sided aortic arch with a normal brachiocephalic branching pattern. The aortic root is normal in size.Pulmonary VeinsAll four pulmonary veins drain normally into the left atrium.Pulmonary ArteryThe main pulmonary artery is normal in size.Venous AnatomyThe SVC and IVC are normal in size and drain normally into the right atrium.PericardiumThere is no significant pericardial disease noted.Extracardiac FindingsThis study is not designed for the specific evaluation of extra-cardiac findings; therefore, the differentiation between artifacts and real extracardiac pathology may be difficult. If clinically indicated, a separate dedicated evaluation should be considered.
1. Normal size left ventricle with normal systolic function (EF 61%), which is improved when compared to the prior study. LV diastolic volumes are similar to the previous study.2. There is persistence of epicardial late gadolinium enhancement in the basal anterolateral and small segment of the mid inferolateral walls, but overall there is less myocardial involvement on this study. 3. Normal size RV with normal systolic function (EF 50%).
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Female, 66 years old, with, and parkinsonism, question of central tremor versus Parkinson's disease or both. Moderately extensive patchy foci of white matter T2 hyperintensity are seen in the bilateral cerebral hemispheres and the pons. No evidence of restricted diffusion is seen. No parenchymal edema or significant generalized mass effect is detected. No abnormal extra-axial collections are seen. There are no findings to suggest acute intracranial hemorrhage. The ventricular system is normal in size and morphology. Overall brain parenchymal volume is within normal limits.
Moderately extensive patchy white matter lesions are seen, predominantly in the cerebral hemispheres. The differential for this finding is broad and would include chronic microvascular ischemic disease, sequelae of demyelination, as well as sequelae of other inflammatory processes and/or vasculitis. No other specific findings are seen to account for the patient's symptoms.
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Many shunt revisions, hydrocephalus, headache, stroke, yearly follow up: evaluate for changes. There are postoperative findings related to right hemispherectomy with an unchanged heterogeneous fluid collection in the right extradural space deep to the craniectomy flap that measures up to approximately 15 mm in thickness and midline shift to the right. The deformed third and lateral ventricles are not significantly changed in appearance. However, there is slight interval decrease in size of some cystic compartments in the left occipital lobe that appear to communicate with ventricular system, while other cystic compartments assocated with the ventricular system appear to be unchanged or perhaps slightly larger, although precise comparison is limited due to differences in head positioning. There is unchanged diffuse confluent cerebral white matter T2 hyperintensity in a large portion of the left hemisphere, particularly in the periventricular region. There is a left transparietal tract, but no shunt catheter is present. There is unchanged posterior deviation and areas of encephalomalacia in the upper cervical spinal cord. There is no evidence of acute intracranial hemorrhage, mass, or acute infarct. The major cerebral flow voids are intact. The orbits, skull, paranasal sinuses, and scalp soft tissues are unchanged.
1. Chronic postoperative findings related to right hemispherectomy with no significant change in the deformed ventricular system and gliotic portions of the left cerebral hemisphere, although cyst compartments in the left cerebral hemisphere that seem to be associated with the ventricular system appear to have fluctuated slightly in size.2. Unchanged posterior deviation and areas of encephalomalacia in the upper cervical spinal cord, which may be attributable to adhesions and chronic infarction, respectively. A dedicated cervical spine MRI may be useful for further characterization.
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58 years Female (DOB:3/5/1958)Reason: primary CNS lymphoma s/p treatment History: please compare with previous MRI in the systemPROVIDER/ATTENDING NAME: CHADI NABHAN CHADI NABHAN The CSF spaces are appropriate for the patient's stated age with no midline shift. The patient is status post burr hole placement along the left parietal calvarium for a previous left parietal lobe stereotactic biopsy.There is confluent signal change present within the left periventricular subcortical white matter centered in the left parietal lobe which has extended further compared to the prior exam. The area involved canal measures 60 x 27 mm axial dimensions and previously measured 47 x 20 mm axial dimensions. There is no associated contrast enhancement. There is susceptibility effect within the left parietal lobe in the location where there was a ring-enhancing lesion on the 9/4/2015 exam.There is a mild degree of periventricular and subcortical punctate hyperintense white matter lesions present identified on the FLAIR and T2 images. Additional T2 and FLAIR punctate hyperintense foci present in the range stem, internal capsules and deep gray nuclei.Normal vascular flow voids are present in the distal carotid and vertebral arteries, the basilar artery and the proximal anterior, middle and posterior cerebral arteries as well as the internal cerebral veins and superior sagittal sinus.The visualized portions of the paranasal sinuses are clear. The visualized portions of the mastoid air cells are clear. The visualized portions of the orbits are intact.
1.Since the prior exam, white matter changes associated with a left parietal lesion have extended further. It is conceivable that this white matter change is related to posttreatment change.2.No enhancing mass lesion is appreciated intracranially to suggest recurrence of the lymphoma.3.Periventricular and subcortical white matter lesions as well as punctate lesions in the deep gray nuclei and brainstem are nonspecific. They are most likely vascular related.
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Male 63 years old with elevated PSA of 30 and two negative biopsies. Evaluate for prostate masses. PELVIS:PROSTATE:Prostate Size: 5.1 x 4.2 x 4.8 cmPeripheral Zone: No suspicious lesion.Central Gland: Benign nodules.Seminal Vesicles: No significant abnormality noted.Extracapsular Extension: None.BLADDER: No significant abnormality noted.LYMPH NODES: No pelvic lymphadenopathy.BONES, SOFT TISSUES: No significant abnormality noted.OTHER: There is a 1.3 x 1.0 cm utricle cyst.
1.Benign prostatic hypertrophy.2.No suspicious prostatic lesion.
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Female 64 years old with right knee pain. Evaluate for right knee meniscal tear. MENISCI: The menisci are intact.ARTICULAR CARTILAGE AND BONE: There is thinning of the articular cartilage in the medial and lateral compartments without evidence of full-thickness defect. The patellar cartilage is thinned and irregular with full-thickness loss over the median facet with underlying reactive marrow change. There is also thinning and irregularity of the cartilage in the femoral trochlea. Other than reactive marrow change, bone marrow signal intensity is within normal limits.There are lateral and tiny medial compartment osteophytes.LIGAMENTS: The cruciate and collateral ligaments are intact. EXTENSOR MECHANISM: The extensor mechanism is intact.ADDITIONAL
1.No evidence of meniscal tear.2.2 loose bodies within the joint.3.Osteoarthritis as described above.
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49-year-old woman with history of metastatic breast cancer, now with lower back pain radiating down the legs bilaterally. There is a nodular enhancing mass involving the conus medullaris and cauda equina roots. The largest of these lesions appears intramedullary and measures 10 x 9 mm in axial dimension and 22 mm in craniocaudal dimension centered at the T12 level. There appears to be associated intraparenchymal invasion, with surrounding edema. Additionally, there are nodular enhancing lesions along the dural surface of the cauda slightly superiorly at the T11/T12 level and involving the left L4 cauda equina roots. In addition, there is amorphous enhancing tumor in the sacral spinal canal, with extension into the right S1/S2 neural foramen. The conus medullaris is situated at L1/L2 level. The vertebral body and intervertebral disc heights are within normal limits. The lumbar spinal alignment is within normal limits. The bone marrow signal is unremarkable. There are slight disc bulges at L3/L4, L4/L5, and L5/S1, but no significant spinal canal or neural foraminal narrowing. The paraspinous soft tissues are within normal limits.
Multiple tumors involving the conus medullaris, cauda equina, and sacral spinal canal are compatible with metastatic disease.I personally reviewed the Images and/or procedure with the Resident/Fellow and agree with this report.
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Migraine without aura, intractable, without status migrainosus [G43.019] / Obesity, unspecified [E66.9], Reason for Study: ^Reason: 46 y.o,. with worsening headaches c/w migraine but hx of cancer - tumor, other mass lesion? History: worsening headache, Brain MRINo evidence of acute ischemic or hemorrhagic lesion.Right parieto-temporal lobe high signal focus on FLAIR images is non specific.The ventricles, sulci and cisterns are symmetric and unremarkable. There is no mass, mass effect, edema, midline shift, intra or extra-axial fluid collection/hemorrhage, restricted diffusion/acute ischemia, or abnormal contrast enhancement. The midline structures and cranial-cervical junction are normal. Normal flow voids are identified in the major intracranial vessels. The mastoid air cells are clear. A small left maxillary sinus retention cyst.Brain MRA3D time of flight MOTSA MRA brain images with maximum intensity projections of the anterior/posterior intracranial circulation demonstrate normal ICAs, MCAs and ACAs. Vertebrobasilar system appears to be normal. Bilateral PCAs are fetal origin.
1. No evidence of acute ischemic or hemorrhagic lesion. No abnormal enhancement.2. Normal brain MRA.
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50 years Female (DOB:9/24/1966)Reason: Chronic LBP without sciatica, + radiculopathy RLE; worsening History: PROVIDER/ATTENDING NAME: SERVICES ANCILLARY SERVICES ANCILLARY Five lumbar type vertebral bodies are presumed to be present which are appropriate in overall alignment and height. The conus medullaris on sagittal imaging is grossly intact. A 7 mm T1 hyperintense well-circumscribed round lesion is present within the L1 vertebral body which most likely represents a hemangioma.At L5-S1 there is no significant compromise to spinal canal or neural foramina.At L4-5 there is no significant compromise to spinal canal or neural foramina. There is bilateral facet hypertrophy present at this level left more than right without significant compromise.At L3-4 there is no significant compromise to spinal canal or neural foramina.At L2-3 there is no significant compromise to spinal canal or neural foramina.At L1-2 there is no significant compromise to spinal canal or neural foramina.
No compromise to lumbar spinal canal or neural foramina.
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Diagnosis: Radiculopathy, lumbar regionClinical question: please do Dr Javed MS protocol and compare to priorSigns and Symptoms: vertigo, headache MRI brain:There is redemonstration of a 4 mm x 5 mm focus of enhancement in the right pons which is hypointense on T1 and was previously hyperintense on FLAIR imaging. On the T2 sagittal cervical spine images it is hyperintense on the STIR T2 images. Susceptibility weighted imaging on the prior exam demonstrates some susceptibility effect.There is a mild degree of periventricular and subcortical white matter lesions present which are asymmetrically more numerous in the left hemisphere relative to the right. Compared to the previous exam these lesions appear somewhat more conspicuous on the current exam but have not changed in number or size. The difference in conspicuity can be accounted for on the basis of slice thickness.The visualized portions of the paranasal sinuses are clear. The visualized portions of the mastoid air cells are clear. The visualized portions of the orbits are intact.MRI cervical spine:The cervical vertebral bodies are appropriate in overall alignment and height. There is mild reversal of the normal cervical curvature present. The cervical spinal cord has normal signal characteristics and overall morphology.At C2-3 there is no significant compromise to the spinal canal or neural foramina.At C3-4 there is no significant compromise to the spinal canal or neural foramina. There is a small central disc protrusion at this level which was also present on the prior examAt C4-5 there is no significant compromise to the spinal canal or neural foramina. There is redemonstration of a small central disc protrusion at this levelAt C5-6 there is no significant compromise to the spinal canal or neural foramina.At C6-7 there is no significant compromise to the spinal canal or neural foramina. There is a small central disc protrusion at this level.At C7-T1 there is no significant compromise to the spinal canal or neural foramina.The vertebral artery flow voids appear to be intact.The left lobe of the thyroid is heterogeneousLumbar spine:Five lumbar type vertebral bodies are presumed to be present which are appropriate in overall alignment and height. The conus medullaris on sagittal imaging is grossly intact. No abnormal enhancing lesions are identified in the lumbar spine. There is a T1 hyperintense focus in the L3 vertebral body which is eccentric towards the right side and measures 11 mm in diameter and most likely represents a vertebral body hemangioma. It suppresses on the inversion recovery images and the fat suppressed images. No abnormal enhancing lesions are appreciated in the spinal canal.At L5-S1 there is no significant compromise to spinal canal or neural foramina. There is mild bilateral facet hypertrophy at this level.At L4-5 there is no significant compromise to spinal canal or neural foramina. There is mild ligamentum flavum hypertrophy at this level. There is disc desiccation and a minor disc bulge at this level.At L3-4 there is no significant compromise to spinal canal or neural foramina. There is some mild loss of disc space height and a minor disc bulge at this level.. There is mild ligamentum flavum hypertrophy at this level.At L2-3 there is no significant compromise to spinal canal or neural foramina.At L1-2 there is no significant compromise to spinal canal or neural foramina.
1.There is a punctate enhancing lesion in the pons. It was also present on the prior exams from 2010 and 2009 and has not changed substantially. It is possible this represents capillary telangiectasia 2.There is a mild degree of periventricular and subcortical white matter lesions present which are nonspecific. Although it is conceivable that these are related to demyelinating disorder at this age they're more likely vascular related based on the imaging appearance and frequency of occurrence.3.There are mild degenerative changes present in the lumbar spine and the cervical spine without significant compromise to spinal canal or exiting nerve roots.4.Heterogeneous left lobe of thyroid is nonspecific finding.
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Right-sided weakness. Acute CVA. Non-enhanced CT of brain:There is evidence of a nonhemorrhagic acute left MCA cortical stroke in the left frontal lobe. There is subtle associated mass effect and effacement of adjacent cortical sulci. No evidence of midline shift.Patchy periventricular foci of low-attenuation is concerning for small vessel ischemic disease of indeterminate age. Follow-up with an MRI is recommended. Ventricular system is within normal range of size for patient's stated age of 70. No abnormalities of basal ganglia, thalami, pons or the cerebellum is detected. Mild vascular calcification of bilateral cavernous carotid are noted. Limited view of orbits, paranasal sinuses and mastoid air cells are unremarkable. Old healed fracture of posterior lateral wall of right maxillary sinus in this limited view is identified.
1.Acute left MCA frontal lobe nonhemorrhagic cortical stroke.2.Small vessel disease of indeterminate age.
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Long-standing knee pain. Status post soccer injury MENISCI: The medial meniscus is normal. Examination of the lateral meniscus reveals a complex tear of the posterior horn with both a vertical and a horizontal component.ARTICULAR CARTILAGE AND BONE: There is a bone contusion in the lateral posterior proximal tibiaLIGAMENTS: The PCL is normal. The medial collateral ligament and the lateral collateral complex are normal.Examination of the anterior cruciate ligament reveals abnormal increased signal on the T2-weighted images. Although some fibers may be intact there is at least a partial tear of the anterior cruciate ligament. EXTENSOR MECHANISM: No significant abnormality noted.ADDITIONAL
Complex tear of the posterior horn of the lateral meniscus. At least a partial tear of the anterior cruciate ligament.
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Images are slightly limited by patient motion. The lumbar spine is in normal alignment, with a normal lumbar lordosis. The vertebral body heights are well-maintained. No worrisome focal marrow signal abnormality is appreciated. There is no pathological enhancement. The distal spinal cord and conus are within normal limits with the conus terminating at the L2 level. No abnormal postcontrast enhancement is visualized. There is developmental narrowing of the lower lumbar spinal canal with prominent dorsal and ventral epidural fat.On sagittal views, T10-T11 and T11-T12 discs demonstrate mild diffuse disc bulges without significant neuroforaminal stenosis or central spinal stenosis.T12-L1 demonstrates a right paracentral disc protrusion causing mild right neural foraminal narrowing without spinal canal stenosis. There is left greater than right ligamentum flavum and facet hypertrophic degenerative change. L1-L2 demonstrates a central disc protrusion causing mild spinal canal stenosis and mild left neuroforaminal stenosis without right neuroforaminal stenosis. Hypertrophic degenerative changes of the facets and ligamentum appears similar to prior examination. L2-L3 demonstrate mild disk disease and mild bilateral facet and ligamentum flavum degenerative changes with associated mild to moderate left neuroforaminal narrowing. There is moderate spinal canal stenosis primarily on the basis of developmental narrowing. L3-L4 demonstrates mild degenerative disk disease with subtle loss of disk height, moderate bilateral facet and ligamentum flavum hypertrophic changes. There is moderate spinal canal stenosis primarily on the basis of developmental narrowing. L4-L5 demonstrates moderate disk disease with loss of disk height and moderate bilateral facet and ligamentum flavum hypertrophic changes. There is a diffuse disc bulge with a right paramedian prominence causing mild to moderate right neuroforaminal stenosis without spinal canal stenosis or left neural foraminal stenosis. There is a right far lateral annular fissure. L5-S1 demonstrates minimal disk disease and moderate bilateral facet and ligamentum flavum hypertrophic changes. No central spinal stenosis or neural foraminal compromise.Degenerative changes of the bilateral sacroiliac joints are partially visualized.
1. No evidence for metastatic disease to the lumbar spine. 2. No significant interval change in multilevel spondylotic changes. Moderate spinal canal stenosis at L2-L3 predominantly on the basis of developmental narrowing with superimposed disc and facet/ligamentous hypertrophic degenerative disease causing mild to moderate left neuroforaminal narrowing.3. There is moderate central spinal canal stenosis at L3-L4 primarily on the basis of developmental narrowing. 4. There is stable right far lateral annular fissure involving the L4-L5 disc with right paramedian prominent disc bulge causing mild to moderate right neuroforaminal stenosis.
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Female, 57 years old, status post resection for cavernoma. Follow-up exam. Findings are seen compatible with left frontal craniotomy and resection of a portion of the left frontal lobe. The resection margin demonstrates a thin rim of diffusion restriction which likely reflects postoperative cytotoxic edema. The surgical cavity contains a mixture of CSF, blood product and debris. Parenchymal edema is evident in the surrounding tissues. The previously demonstrated cavernous malformation is not identified on this examination and has therefore likely been included within the resection. Elsewhere, a few scattered nonspecific foci of FLAIR hyperintensity are seen. No other areas of edema or mass effect are detected. Ventricular size and morphology remain within normal limits.
Expected post operative findings are seen compatible with resection of a left frontal cavernous malformation.
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Clinical question: Evaluate for stenosis. Signs and symptoms: Pain. Nonenhanced cervical MRI:There is normal anatomical alignment of vertebral column. There is mild straightening of cervical lordosis likely secondary to degenerative disease.Foramen magnum is unremarkable.C2-C3 is unremarkable.C3-C4 is unremarkable.C4-C5 demonstrate mild degenerative changes without spinal stenosis or neural foraminal compromise.C5-C6 demonstrate moderate disc disease and loss of disc height and mild facet disease. There is moderate (left greater than right) neural foraminal compromise and no central spinal stenosis.C6-C7 demonstrate advanced disc disease and loss of disc height. There is a disc-osteophyte complex in the midline and to the right. There is resultant significant right neural foraminal compromise, moderate left neural foraminal compromise and no central spinal stenosis.C7-T1 is unremarkable.Upper most visualized thoracic spine to T3 level demonstrate no spinal stenosis.
1.At C6-C7 degenerative changes and including a disc-osteophyte complex results in significant bilateral (right greater than left) neural foraminal compromise and no central spinal stenosis.2.At C5-C6 degenerative changes results in moderate bilateral neural foraminal compromise (left greater than right) and no central spinal stenosis.3.Mild degenerative changes at other levels as detailed4.Normal signal intensity and caliber of cervical and upper most visualized thoracic cord.
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Pain. Cuff tear? Mild osteoarthritis affects the glenohumeral and acromioclavicular joints. Scattered calcific densities along the greater tuberosity and within the acromiohumeral interval likely reflect calcific tendinosis. The acromiohumeral interval is preserved, but please note that the previous MRI exam showed a full-thickness rotator cuff tear. Glenohumeral joint alignment is within normal limits. Degenerative arthritic changes affect the visualized thoracic spine. Orthopedic fixation of the cervical spine is incompletely imaged on this study.
Osteoarthritis and other findings as described above.
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Male 64 years old with prostate cancer. Biopsy showed Gleason 3+4 =7 in 4 of 6 cores. The positive finding was on the left mid, left apex, right base and right mid lobes. Evaluation is limited due to artifact from metallic hardware.PELVIS:PROSTATE:Prostate Size: 4.0 x 3.2 cmPeripheral Zone: There are left mid and left apex lesions. The largest is in the left apex and measures 6 x 4 mm. It is dark on T2 and ADC. No lesion is seen on the right. There is no extracapsular extension.Central Gland: Multiple benign nodules are noted.Seminal Vesicles: No significant abnormality noted.Extracapsular Extension: None.BLADDER: No significant abnormality noted.LYMPH NODES: No pelvic lymphadenopathy.BONES, SOFT TISSUES: Artifact from bilateral hip arthroplasties limits evaluation of the bones and soft tissues of the pelvis.OTHER: No significant abnormality noted.
1.Limited evaluation due to artifact from metallic hardware.2.Left mid and left apex lesions are compatible with prostate carcinoma. No lesion is seen on the right. 3.No extracapsular extension or pelvic lymphadenopathy.
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22-year-old male with pain. Evaluate patellofemoral osteochondral defect. MENISCI: The medial meniscus appears intact. The lateral meniscus appears intact.ARTICULAR CARTILAGE AND BONE: There is a focus of intermediate to high signal intensity within the articular cartilage of the patella, centrally, indicating focal degeneration, measuring approximately 8 mm in diameter. There is a small focus of signal abnormality, with a depth of approximately 2 to 3 mm, within the underlying subchondral bone with adjacent bone marrow edema. These findings are compatible with the stated history of an osteochondral defect. There is relative sparing of the articular cartilage of the medial and lateral compartments.LIGAMENTS: The cruciate and collateral ligaments appear intact. EXTENSOR MECHANISM: The extensor mechanism appears intact.ADDITIONAL
Central osteochondral defect of the patella and other findings as described above.
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History of left temporal lobe from meningioma resection, auditory and visual hallucinations, suspicious for encephalitis. No evidence of acute ischemic or hemorrhagic lesion.There is about 4mm sized intensely enhancing area (series 901, image 113/300) on the right basal ganglia, likely globus pallidus on enhancement. However, this is the only abnormal enhancement on this scan. Therefore, it is likely to be a vascular enhancement such as focal dilated venous structure. Possibility of arterial aneurysm is low.Therefore, if clinically indicated, follow up MRI with contrast enhancement can be considered.Redemonstration of left temporal lobe anterior aspect large resection cavity with the surrounding gliosis indicating postoperative changes. These are showing no interval changes since prior scan.Patch high signal intensities on FLAIR images on bilateral periventricular white matter indicating minimal to mild nonspecific small vessel ischemic disease, no change since prior scan.The ventricles, sulci and cisterns are symmetric and unremarkable. The midline structures and cranial-cervical junction are normal. Normal flow voids are identified in the major intracranial vessels. The paranasal sinuses and mastoid air cells are clear.
1. No evidence of acute ischemic or hemorrhagic lesion. 2. Focal intensely enhancing area on the right basal ganglia which likely represent vascular structure such as dilated venous structure. 3. Post resection status of the left temporal area meningioma with post operative changes, no interval change since prior exam.4. Non specific small vessel ischemic disease. No change since prior exam.
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Diagnosis: Transient alteration of awarenessClinical question: evaluate for brain metsSigns and Symptoms: altered mental status The CSF spaces are appropriate for the patient's stated age with no midline shift. No focus of diffusion restriction is identified in the brain parenchyma.There is a mild to moderate degree of periventricular and subcortical punctate hyperintense white matter lesions present identified on the FLAIR and T2 images. There as several punctate T2 and FLAIR hyperintense brainstem lesions present.No abnormal enhancing mass lesions are appreciated intracranially. No intracranial hemorrhage is identified. No edema is identified within the brain parenchyma.Normal vascular flow voids are present in the distal carotid and vertebral arteries, the basilar artery and the proximal anterior, middle and posterior cerebral arteries as well as the internal cerebral veins and superior sagittal sinus.The visualized portions of the paranasal sinuses demonstrate some mucosal thickening. The visualized portions of the mastoid air cells are clear. The visualized portions of the orbits are intact.
1.Periventricular and subcortical white matter changes of a mild to moderate degree are nonspecific. At this age they are most likely vascular related. To a lesser degree there are similar appearing brainstem lesions present also most likely vascular related.2.No intracranial mass lesion is identified.
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There is no evidence of intracranial hemorrhage, mass, or acute infarct. There are no areas of abnormal parenchymal signal. The ventricles and basal cisterns are normal in size and configuration. There is no midline shift or herniation. The major cerebral flow voids are intact. The skull, paranasal sinuses, and scalp soft tissues are unremarkable. The midline structures and craniocervical junction are within normal limits.
Unremarkable brain MRI.
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History of left renal lesion seen on ultrasound. ABDOMEN:LIVER, BILIARY TRACT: The liver dome was not included in the axial images. The liver is otherwise normal in morphology signal intensity and enhancement without a suspicious lesion. No biliary ductal dilatation. Normally distended gallbladder.SPLEEN: No significant abnormality noted.PANCREAS: No significant abnormality noted.ADRENAL GLANDS: No significant abnormality noted.KIDNEYS, URETERS: The right kidney is located in the pelvis with punctate subcentimeter simple cysts.Orthotopic left kidney with a dorsal interpolar 1.4 cm minimally complex cyst with layering proteinaceous/hemorrhagic fluid and no suspicious postcontrast enhancement, corresponding to the cyst seen on ultrasound. Additional too small to characterize punctate probable benign cysts. No hydroureteronephrosis.RETROPERITONEUM, LYMPH NODES: No significant abnormality noted.BOWEL, MESENTERY: No significant abnormality noted.BONES, SOFT TISSUES: No significant abnormality noted.OTHER: No significant abnormality noted.
The left renal lesion seen on ultrasound corresponds to a minimally complex benign proteinaceous/hemorrhagic cyst without suspicious postcontrast enhancement.
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New onset headache and dizziness. There is no evidence of intracranial hemorrhage, mass, or acute infarct. There is confluent periventricular white matter T2 hyperintensity and a few scattered deep white matter T2 hyperintensity foci. There is no abnormal intracranial enhancement. There is perhaps mild diffuse cerebral volume loss. There is a mega cisterna magna. There is no midline shift or herniation. The major cerebral flow voids are intact. The orbits, skull, and scalp soft tissues are grossly unremarkable. There are scattered paranasal sinus small retentions cysts, including adjacent to the left nasolacrimal duct.
Perhaps mild diffuse cerebral volume loss and nonspecific areas of cerebral white matter signal abnormality may represent chronic small vessel ischemic disease, for example. Otherwise, no evidence of intracranial hemorrhage, mass, or acute infarct.
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Clinical question: Structural lesion causing headache. Signs and symptoms: Diffuse sharp headache with left sharp trigeminal distribution pain. Pre-and enhanced brain MRI:Negative diffusion weighted images.Examination demonstrates a few punctate foci of nonspecific flair hyperintensity in the subcortical and periventricular white matter bilateral seen hemispheres. Although nonspecific in proper clinical setting these findings could represent mild chronic small vessel ischemic strokes.The anatomical morphology as well as the signal intensity of brain parenchyma is otherwise entirely within normal on all MRI sequences. Unremarkable cerebral cortex, cortical sulci, ventricular system, CSF spaces and brain myelination.There is no detectable abnormal parenchymal or leptomeningeal enhancement. The signal 80 the major intracranial arterial branches are identified.The signal intensity intracranial venous sinuses are within normal and with normal pattern of enhancement. Calvarium and soft tissues of the scalp are unremarkable and without abnormal enhancement.Unremarkable images through the orbits and including axial fat sat post enhanced series.Paranasal sinuses and bilateral mastoid air cells/middle ear cavities demonstrate normal pneumatization signal.
1.Negative diffusion weighted images.2.Few nonspecific punctate foci of flair hyperintensity the the subcortical and periventricular white matter which in proper clinical setting clips are present minimal chronic small vessel ischemic strokes.3.Unremarkable pre-and post enhanced brain MRI otherwise.4.Unremarkable images through the orbits, paranasal sinuses and well pneumatized mastoid air cells and middle ear cavities.
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52 years Female (DOB:12/11/1963)Reason: eval for primary CNS lymphoma, PML, toxoplasma encephalitis, or other CNS malignancy or infection History: HIV, gait instability, cognitive impairment, recently started HART, hx "brain cancer"PROVIDER/ATTENDING NAME: GEORGE W WEYER GEORGE W WEYER There is redemonstration of abnormal signal in the right cerebellar hemisphere white matter without associated contrast enhancing lesion. It is associated with T2 and FLAIR signal hyperintensity and T1 signal hypointensity with involvement of the white matter of the right cerebellar hemisphere and the right middle cerebellar peduncle. This is stable since the prior exam.There are patchy foci of T2 and FLAIR hyperintensity in the medulla, pons and lower midbrain. This is stable since the prior exam.The CSF spaces are appropriate for the patient's stated age with no midline shift. There is a mild degree of periventricular and subcortical punctate hyperintense white matter lesions present identified on the FLAIR and T2 images.There is a small focus of susceptibility effect present adjacent to the frontal horn of the left lateral ventricle. It is not seen on any of the other pulse sequences.No abnormal enhancing mass lesions are appreciated intracranially.Normal vascular flow voids are present in the distal carotid and vertebral arteries, the basilar artery and the proximal anterior, middle and posterior cerebral arteries as well as the internal cerebral veins and superior sagittal sinus.The visualized portions of the paranasal sinuses demonstrate some small opacities. The visualized portions of the mastoid air cells are clear. The visualized portions of the orbits are intact. The nasopharyngeal adenoids are large which could be a manifestation of HIV.
1.There is a right cerebellar white matter lesion present. Differential considerations may include demyelinating focus including PML. Other lack of contrast enhancement makes lymphoma and toxoplasmosis less likely these diagnosis cannot be entirely excluded.2.Periventricular and subcortical white matter signal changes of a mild to moderate degree are present which are nonspecific. They could be vascular related, related to demyelination, trauma, vasculitis, sarcoid. They are nonspecific. 3.There are patchy lesions present in the brainstem which are nonspecific.4.There is a microhemorrhage present adjacent to the frontal horn of the left lateral ventricle. It is of unclear significance in isolation.
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Right foot ulcer There is subcutaneous ulceration overlying the head of the fifth metatarsal. There is abnormal low T1 marrow signal and increased T2 marrow signal within the head of the fifth metatarsal consistent with osteomyelitis. There is overlying subcutaneous edema throughout the foot. There is no discrete focal fluid collection identified. There is moderate degenerative changes of the midfoot. The remaining marrow signal is otherwise normal.
Findings consistent with osteomyelitis of the head of the fifth metatarsal.
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Evaluate for lateral meniscal tear. Knee pain with sports injury one month ago, with stiffness. MENISCI: No significant abnormality noted.ARTICULAR CARTILAGE AND BONE: We see no articular cartilage deformity or bone marrow edema.LIGAMENTS: There is abnormal thickening and increased signal intensity of the anterior cruciate ligament, particularly involving the posterior and proximal fibers. This is concerning for a tear, at least involving the posterolateral bundle, but we cannot exclude a complete tear of the fibers of the proximal ligament. This may represent subacute injury given lack of bone marrow edema. Mucoid degeneration of the ligament is considered less likely. The posterior cruciate, lateral collateral and medial collateral ligaments are intact.EXTENSOR MECHANISM: No significant abnormality noted.ADDITIONAL
Abnormal thickening and increased signal intensity of the anterior cruciate ligament is suggestive of at least a partial thickness tear despite absence of bone contusions and joint effusion. We see no meniscal tear.
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Clinical question: Stroke. Signs and symptoms: Right-sided weakness. Nonenhanced CT of brain:Subacute nonhemorrhagic right cerebellar and right medullary region in the distribution of right pica stroke is again identified. There is only subtle mass effect with effacement of sulci and no evidence of mass effect on the fourth ventricle.Well demarcated nonhemorrhagic lacunar infarct of right thalamus as was noted on prior MRI exam.Small vessel disease of indeterminate age is subcortical white matter of bilateral cerebral hemispheres (left greater than right). Overall this appearance also is similar to prior MRI examination. No evidence of hemorrhage.CTA of the cervical region:Right carotid, circumferential plaque at the origin of right internal carotid artery with no hemodynamically significant stenosis is noted. The right common carotid artery including its origin and the rest of the cervical portion of right internal carotid artery is unremarkable.Left carotid, circumferential complex plaque at the origin of left internal right artery with no minimal calcification is noted. This results in significant high-grade stenosis of left internal carotid artery at this site. The left common carotid artery and including its origin and the rest of the cervical portion of the left internal carotid artery is unremarkable and widely patent.Right vertebral artery is small in caliber and is believed to represent a non-dominant vertebral (and normal anatomical variation). There is no evidence of a stenotic lesion.Left vertebral artery, there is a non-calcific circumferential plaque at the origin of the dominant the left vertebral artery is noted. There appears to be more than 50% stenosis at this site. The rest of left vertebral artery is unremarkable.Limited view of lower tic origin the origin of major vessels are essentially unremarkable.CTA of intracranial circulation:Carotid system, patent bilateral supraclinoid internal carotid arteries. Minimal atherosclerotic irregularities noted.Middle cerebral arteries and their branches demonstrate mild atherosclerotic disease however but no evidence of any large vessel vascular occlusion or high-grade stenosis.Bilateral anterior cerebral arteries demonstrate multiple foci of high-grade stenosis and ectatic changes. Findings are secondary to atherosclerotic disease. Vertebral basilar system, diffuse atherosclerotic disease of the basilar artery with multi-level areas of mild vascular lumen compromise. Similar findings are noted in the intracranial component of dominant left vertebral artery in particular in its distal component.The right vertebral artery is the nondominant vessel. There is discontinuity of the distal component of the right vertebral artery. This represents occlusion of this vessel proximal to its junction with the basilar artery. The very distal portion of right vertebral artery is visualized and shows significant decrease in its caliber to its patent more proximal component.
1.Revisualization of multiple small vessel strokes, lacunar strokes and a right cerebellar -- medullary stroke in the distribution of right pica branch. No evidence of hemorrhagic transformation.2.Atherosclerotic plaque with minimal calcification however no hemodynamically significant stenosis at the origin of right internal carotid origin.3.Significant atherosclerotic disease of the left internal carotid artery origin with very high-grade stenoses.4.More than 50% stenosis at the origin of the dominant left vertebral artery and otherwise unremarkable vertebral arteries bilaterally in the neck.5.Atherosclerotic disease of supraclinoid internal carotid arteries, bilateral middle cerebral arteries with areas of mild to moderate vascular compromise. Atherosclerotic disease results in high-grade stenosis and ectatic changes of bilateral anterior cerebral arteries.6.Patent dominant left vertebral artery intracranially with minimal atherosclerotic disease.7.Patent basilar artery however but extensive atherosclerotic disease and mild vascular lumen compromise.8.Complete occlusion of the mid section of the intracranial component of the nondominant right vertebral artery. There is significant decrease in the caliber of visualized very distal right vertebral artery compared to patent a proximal component. If further evaluation is required for management a conventional angiogram would improve detection and the cause of occlusion and morphology of this vessel evaluation.
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72-year-old female with decreased vision. Evaluate for etiology of retinal edema. MRI brain:There is no evidence of intracranial hemorrhage, mass, or acute infarct. There is mild progression of the periventricular and subcortical T2/FLAIR hyperintensities which is nonspecific but likely related to small vessel ischemic disease. There is no abnormal intracranial enhancement. The ventricles and basal cisterns are normal in size and configuration. There is no midline shift or herniation. The major cerebral flow voids are intact. The skull, paranasal sinuses, and scalp soft tissues are grossly unremarkable.MRI orbits: Motion limited exam.There is abnormal bilateral signal and thickening along the posterior aspect of the globes with T2 hyperintensity and mild T1 heterogeneity but no abnormal susceptibility to indicate hemorrhage. The bilateral nature and configuration is suggestive of bilateral retinal attachment. The optic nerves are normal in size and signal intensity, and are symmetric bilaterally. No retrobulbar mass, chiasmatic mass, or parasellar abnormality is seen. Extraocular muscles are unremarkable.
1.Findings suspicious for bilateral retinal detachment. Please correlate with an ophthalmoscopic exam.2.No evidence of intracranial hemorrhage, mass, or acute infarct. 3.Periventricular and subcortical white matter lesions of a mild degree are nonspecific. At this age they are most likely vascular related. This has progressed mildly since the prior exam from 12/2008
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Clinical question: DBS planning. Signs and symptoms: DBS planning Pre and post enhanced brain MRI:Examination is limited and performed utilizing surgical planning protocol and is not a true diagnostic exam.There are also no prior exams for comparison.Examination demonstrates uniform prominence of cortical sulci and supratentorial ventricular system without radiation of midline.There is no detectable abnormal enhancement of parenchyma or the leptomeninges.The signal void of major intracranial arterial branches are identified and there is normal enhancement of intracranial venous sinuses. There is no detectable abnormal signal intensity on T2 or susceptibility MRI sequences.
Pre- and post enhanced surgical planning MRI study as detailed.
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Central sleep apnea with dropped breaths, hypotonia, developmental delay. Evaluate for atrophy vs mass vs other processes explaining clinical condition. There is increased crowding of the foramen magnum compared to the previous exam with pointing of the tonsils. The tonsils descend to the level of the posterior arch of C1 which is compatible with Chiari type I malformation. There is symmetric interval increase in size of the ventricles with proportionate increase in size of the sulci/subarachnoid spaces. Given that these are proportionally increased, this is favored to be secondary to parenchymal volume loss.There is normal myelination pattern for age. There are no focal lesions and no obvious structural abnormalities. The orbits, skull, paranasal sinuses, and scalp soft tissues are grossly unremarkable.
1.Findings compatible with Chiari Type I malformation.2.Symmetrically increased ventricular size and sulci/subarachnoid spaces suspicious for global parenchymal volume loss.3.Normal myelination pattern for age.
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Clinical question: Evaluate interval enlargement of possible frontal meningioma. Signs and symptoms: CTH with enlarged possible meningioma. Nonenhanced brain MRI:No acute intracranial process and negative diffusion weighted series.Examination demonstrates a dural based extra-axial mass in the anterior left middle cranial fossa along the inner table of the great wording of sphenoid. It measures at 32 x 17 mm in transaxial dimensions (axial T2 series 6 image 19). There is resultant mass effect and posterior displacement of left temporal tip however without detectable FLAIR or T2 signal abnormality to suggest vasogenic edema. The location and signal intensity of the finding is suggestive of a meningioma. No contrast was given.Additionally examination demonstrates scattered periventricular and subcortical as well as bilateral basal ganglia and minimally pontine foci of FLAIR hyperintensity which considering patient's stated age of 77 likely representing chronic nonhemorrhagic small vessel ischemic strokes of moderate degree.The signal intensity of cerebral cortex is within normal.Cortical sulci and ventricular system as well as the CSF spaces are otherwise unremarkable. The signal void of major intracranial arterial branches are identified.Signal intensity of intracranial venous sinuses are unremarkable.Mild mucosal thickening of all visualized paranasal sinuses are noted. Bilateral mastoid air cells and middle ear cavities demonstrate normal pneumatization signal patterns.
1.Dural based extra-axial mass in the left anterior middle cranial fossa presumed a meningioma is again noted. Subtle mass effect on the left anterior temporal tip without vasogenic edema or midline shift.2.Negative diffusion weighted images and findings suggestive of mild to moderate chronic nonhemorrhagic small vessel ischemic strokes are noted.
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57-year-old female with history of sarcoma. Please evaluate for recurrence and extent of disease. ABDOMEN:LIVER, BILIARY TRACT: No significant abnormality noted.SPLEEN: No significant abnormality noted.PANCREAS: No pancreatic ductal dilatation. Punctate T2 hyperintense focus of the inferior pancreatic body (coronal series 4 image 23) is unchanged.ADRENAL GLANDS: No significant abnormality noted.KIDNEYS, URETERS: Status post right nephrectomy. Small simple cysts of the left kidney. No hydronephrosis.RETROPERITONEUM, LYMPH NODES: Stable soft tissue nodule adjacent to the medial aspect of the right diaphragmatic crus measuring 2.1 x 1.3 cm (series 9 image 32) (prior 2.2 x 1.2 cm). Enhancement is most evident on the delayed series.There is a new fat signal intensity lesion of the right posterior diaphragmatic crus measuring 1.7 x 2.7 cm (series 7 image 41). This lesion is hyperintense on the T2 fat saturated sequence (series 9 image 42). Peripheral enhancement is noted on the delayed postcontrast sequence (series 13 image 463).BOWEL, MESENTERY: Status post right hemicolectomy with ileocolonic anastomosis.Adjacent to the ileal colonic anastomosis, there is a new 5.4 x 4.9 cm T2 hyperintense lesion (coronal series 4 image 23) with fat signal intensity. Hyperintense signal intensity is noted on the fat saturated T2 sequence (series 9 image 44). Mild peripheral enhancement is seen on the delayed postcontrast sequence (series 13 image 455).BONES, SOFT TISSUES: No significant abnormality noted.OTHER: Stable small cardiophrenic angle lymph node.
1.New 5.4 x 4.9 cm lesion adjacent to the ileocolonic anastomosis and a new 1.7 x 2.7 cm lesion of the posterior right diaphragmatic crus. These lesions demonstrate fat signal intensity and peripheral enhancement on the delayed series. These findings are concerning for liposarcoma recurrence.2.Stable right retroperitoneal soft tissue nodule adjacent to the right diaphragmatic crus medially.
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68-year-old male with history of right renal cyst. ABDOMEN:LUNG BASES: No significant abnormality notedLIVER, BILIARY TRACT: Cholelithiasis. Scattered T2 hyperintense non-enhancing lesions compatible with benign cysts.SPLEEN: Small splenule. PANCREAS: No significant abnormality notedADRENAL GLANDS: No significant abnormality notedKIDNEYS, URETERS: Right lower pole cystic lesion containing areas of intrinsic increased T1 signal without enhancement measuring 2.6 x 2.4 cm, not significantly changed dating back to 2013. Additional benign appearing exophytic subcentimeter cystic lesions are present bilaterally.RETROPERITONEUM, LYMPH NODES: No significant abnormality noted.BOWEL, MESENTERY: No significant abnormality noted.BONES, SOFT TISSUES: No significant abnormality notedOTHER: No significant abnormality noted
Benign cyst in the right lower pole, stable in size from 2013, probably containing proteinaceous or mineral debris. Other scattered subcentimeter lesions also have a benign appearance.
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Male 57 years old Reason: hx of portal vein thrombosis, cirrhosis, and HCC History: eval for portal vein thrombosis LIMITED ABDOMENLIVER: Heterogeneous liver. Coarse echotexture of the liver. There is partial main portal vein thrombus. Right portal vein is not well visualized. Ill-defined masses in the right and left lobe of the liver that were seen on CT are not well seen on ultrasound. These lesions were suspicious for hepatocellular carcinoma. Further evaluation of the liver with MRI is recommended.BILIARY TRACT: No evidence of intra or extrahepatic biliary dilatation. Status post cholecystectomy.PANCREAS: No significant abnormalities noted.SPLEEN: Spleen is enlarged measuring 16 cm. RIGHT KIDNEY: No significant abnormalities noted.OTHER: No significant abnormalities noted.
Cirrhotic liver. Infiltrative, ill-defined bilateral lobar liver masses detected on the previous CT were not well seen on today's study. These lesions were suspicious for hepatocellular carcinoma. Further evaluation with liver MRI is recommended.Partial thrombosis of the main portal vein.Splenomegaly.
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58 years Female (DOB:5/20/1957)Reason: lung mets to brain s/p SRS To L temporal and R frontal met and most recently whole brain radiation History: eval for extent of diseasePROVIDER/ATTENDING NAME: STEVEN J CHMURA STEVEN J CHMURA Since the prior exam multiple brain parenchymal lesions have increased in size. One in the posterior aspect of the left temporal lobe previously measured 7 x 7 mm now measures 12 x 12 mm axial dimensions. One in the left cerebellar hemisphere previously measured 10 mm and now measures 21 x 15 mm. One adjacent to the trigone of the left lateral ventricle was barely visible on the prior exam and now measures 9 x 12 mm. One in the right frontal lobe was not present on the prior exam measures 4 mm. One in the right middle frontal gyrus measures 12 mm and previously measured 3.5 mm. One adjacent to the the right precentral sulcus in the right precentral gyrus measures 6 mm and previously measured 2 mm. There is edema present in the posterior fossa associated with the left cerebellar lesion which partially distorts the fourth ventricle and mildly crowds the posterior fossa.Normal vascular flow voids are present in the distal carotid and vertebral arteries, the basilar artery and the proximal anterior, middle and posterior cerebral arteries as well as the internal cerebral veins and superior sagittal sinus.The visualized portions of the paranasal sinuses are clear. The visualized portions of the mastoid air cells demonstrate scattered opacities. The visualized portions of the orbits are intact.
1.Since the prior exam patient's metastatic lesions have increased in size . In addition there are a couple new brain metastatic lesions.2.There is more mass effect in the posterior fossa the current exam relative to the prior exam which is related to vasogenic edema from a metastatic lesion.
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Left ear tinnitus and sensorineural hearing loss. . There is apparent deficiency of bone overlying the left superior semicircular canal. The rest of the inner ear structures otherwise appear unremarkable. The bilateral cranial nerve 7 and 8 complexes are intact. There is no evidence of mass lesions. The bilateral mastoid air cells and middle ears also appear unremarkable. A subcentimeter focus of high T1 signal along the midline of the anterior cranial fossa may represent prominent fatty marrow within the crista galli rather than a meningioma, although this is incompletely characterized.
1. Apparent left superior semicircular canal dehiscence, which can be confirmed via a temporal bone CT, if clinically warranted. Otherwise, no evidence of vestibular schwannoma.2. A subcentimeter focus of high T1 signal along the midline of the anterior cranial fossa may represent prominent fatty marrow within the crista galli rather than a meningioma, although this is incompletely characterized.
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There is mild exaggeration of the lumbar lordosis without sagittal spondylolisthesis. There is mild loss of height of the T12, L1, L2, and L4 vertebral bodies overall worse compared to the 12/31/2011 MRI, but appearing similar to the more recent 11/24/2014 CT. There are additional mild endplate deformity/Schmorl's nodes nodes involving T12-L5 which also appear similar to 11/24/2014 CT. There is no significant bone marrow edema to suggest acute compression fracture. The bone marrow is mildly heterogenous including small foci of decreased T1 and T2 signal within the L2 vertebral body and within the left sacrum. The focus in the L2 vertebral body appears unchanged from the 12/31/2011 exam. These areas do not demonstrate associated increased STIR signal to suggest edema and favored to be benign, although remain nonspecific. No clearly destructive osseous lesions are identified. There is mild loss of disc height at L1-L2. The T11-L2 discs are desiccated. The conus terminates at L1-L2. The paravertebral soft tissues are unremarkable. Individual levels as below:L1-L2: Mild disc bulge without significant central canal or foraminal stenosis.L2-L3: No significant central canal or foraminal stenosis.L3-L4: Mild disc bulge without significant central canal or foraminal stenosis.L4-L5: Mild disc bulge. Mild facet hypertrophy and ligamentum flavum thickening. Mild central canal stenosis. Minimal bilateral foraminal stenosis.L5-S1: No significant central canal or foraminal stenosis.
1.Multiple chronic mild vertebral body compression deformities without bone marrow edema to suggest acute fracture.2.Mild spondylosis as described above including mild central canal stenosis at L4-L5.3.Mild facet arthropathy, relatively worse at L4-L5 which may be contributing to patient's low back pain.
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Reason: eval mass History: R proximal humerus mass Within the superficial soft tissues overlying the right deltoid and biceps brachii muscle, there is a homogeneous 7 x 3 x 2 cm mass with well-defined margins and with signal characteristics identical to subcutaneous fat on all sequences. A thin capsule and a few thin internal septae are appreciated. The underlying muscles are uninvolved. Bone marrow signal intensity is within normal limits. No axillary lymphadenopathy.
Superficial lipoma within the lateral aspect of the right shoulder.
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79-year-old female with hypertension now with progressive lower extremity weakness x 1 day. Generalized weakness x 2 weeks. No objective neuro findings on exam. Question acute ischemia. Question subdural hematoma. Patient has very poor gait. Patchy areas of deep subcortical and periventricular white matter hypodensity likely represent moderate small vessel ischemic disease, age indeterminate by CT. However, if there is concern for an acute stroke, an MRI is recommended for further evaluation. There is no evidence of intracranial hemorrhage, mass or midline shift. Prominence of the sulci and ventricles indicates mild to moderate corticomedullary volume loss.The calvaria and skull base are radiographically normal. The visualized paranasal sinuses and mastoid air cells are normally pneumatized.
Small vessel ischemic disease, age indeterminate. If there is concern for an acute stroke, an MRI is recommended for further evaluation.
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Left lower extremity weakness, bowel and bladder incontinence. History of metastatic breast cancer. There is extensive T2 hyperintensity involving the thoracic cord extending from the C7 to the T4 levels with mild cord expansion. There is a T2 hypointense intramedullary lesion at the T1 level measuring approximately 5 mm, previously approximately 28 mm in the craniocaudal dimension.Degenerative changes are seen in the cervical spine with disc osteophyte complexes at the C4-C5, C5-C6, and C6-C7 levels. There is minimal retrolisthesis at C5 on C6. Mild cervical spinal canal narrowing related to degenerative disease. Vertebral body heights and alignment in the cervical spine are otherwise maintained.In the thoracic spine at the T6-T7 level there is disc extrusion which appears less prominent than before. There is mild degree of spinal canal stenosis at this level. Possible T2 signal abnormality at this level, sagittal STIR image 7 but appears less severe than before. Vertebral body heights and alignment in the thoracic spine are otherwise maintained.In the lumbar spine, again seen is mild loss of height at the L2 level compatible with a chronic compression fracture. Vertebral body heights and alignment in the lumbar spine are otherwise maintained. Mild degenerative changes throughout the lumbar spine are also seen without significant spinal canal stenosis. There is severe loss of disc height at the L5-S1 level on a degenerative basis. Mild to moderate L5-S1 neural foraminal stenosis.
1. Intramedullary lesion at the T1 level highly suspicious for cord metastasis is decreased in size, currently measuring 5 mm, previously 28 mm in the craniocaudal dimension on prior study from 12/8/2014. Surrounding edema is also decreased in the interval.2. Disc extrusion at the T6-T7 level appears less prominent than 12/8/2014. There is possible T2 signal abnormality in the cord at this level but not well evaluated without axial images. There was definite cord signal abnormality at this level previously, which was presumably related to the extensive edema from the T1 metastases. There is mild degree of spinal canal stenosis at this level. 3. Please note this is a limited exam per cord compression protocol. Consider dedicated total spine MRI with gadolinium to better assess the extent of metastatic disease.Dr. Ali discussed findings with Dr. Jacobs at 1130 hrs on 8/26/2015.
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58 year old female with non small cell lung cancer with new mass seen on the atrial septum on TTE. She also has shortness of breath and chest pain. MRI evaluation for atrial septal mass. Left VentricleThe left ventricle is normal in size with normal systolic function. The overall LV ejection fraction is 56%. The LVEDV is 73 ml (normal range 109+/-23), LV end diastolic volume index is 45 ml/m2 (normal range: 65+/-11), LVESV is 18 ml (normal range 31+/-10), and LV end systolic volume index is 11 ml/m2 (normal range 18+/-5). There are no regional wall motion abnormalities present. There is no late gadolinium enhancement to suggest the presence of an underlying fibrosing, infiltrative, or inflammatory process.There is no myocardial iron overload. There is no LV thrombus. Left AtriumThe left atrium is normal in size.Right VentricleThe right ventricle is normal in size with normal systolic function. The overall RV ejection fraction is 53%, the RV end diastolic volume index is 62 ml/m2 (normal range 69+/-14), the RVEDV is 101 ml (normal range 110+/-24), the RV end systolic volume index is 29 ml/m2 (normal range 22+/-8), and the RVESV is 46 ml (normal range 35+/-13). Right AtriumThe right atrium is mildly dilated. Aortic ValveThe aortic valve is trileaflet, opens widely and there is no significant aortic regurgitation.Mitral ValveThe mitral valve opens widely and there is mild mitral regurgitation.Pulmonic ValveThe pulmonic valve opens widely. There is no significant pulmonic regurgitation.Tricuspid ValveThe tricuspid valve opens widely. There is mild tricuspid regurgitation.AortaThere is a left sided aortic arch with a normal brachiocephalic branching pattern. The aortic root is normal in size.Pulmonary VeinsPulmonary veins drain normally into the left atrium, LUPV poorly visualized.Pulmonary ArteryThe main pulmonary artery is normal in size. Venous AnatomyThe SVC and IVC drain normally into the right atrium. PericardiumThere is a small pericardial effusion.Extracardiac FindingsThere is a large right sided pleural effusion. There is also a large loculated fluid collection at the left lung base. Extensive L lung changes c/w recent CT (post surgical, radiation changes)This study is not designed for the specific evaluation of extra-cardiac findings; therefore, the differentiation between artifacts and real extracardiac pathology may be difficult. If clinically indicated, a separate dedicated evaluation should be considered.
1.Normal sized left ventricle with normal systolic function.2.Normal sized right ventricle with normal systolic function.3.Large right sided pleural effusion. 4.Large loculated fluid collection at the left lung base. 5.No intracardiac mass to explain PET uptake at the aortic root / interatrial septum6.Posterior extracardiac mass noted on TTE is a large loculated L pleural effusion.I personally reviewed the Images and/or procedure with the Resident/Fellow and agree with this report.
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Clinical question: CVA. Signs and symptoms: Headaches and hypertension Nonenhanced CT of brain:There is no definitive evidence of intracranial hemorrhage, edema, mass-effect, midline shift or hydrocephalus. Cortical sulci, ventricular system, CSF cisterns and gray -- white matter differentiation is within normal. Follow-up with an MRI is recommended if clinical concern for stroke in our system. Non-infused CT can this area also the small strokes.Calvarium is intact. Limited view of paranasal sinuses and mastoid air cells are unremarkable.
No definitive evidence of abnormality. Follow-up with an MRI is recommended if clinical concern for stroke persists.
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47 year old with known cardiac sarcoid and history of premature ventricular contraction and nonsustained ventricular tachycardia presenting with palpitations. Left VentricleThe left ventricle is normal in size and systolic function. The overall LV ejection fraction is 63%, the LV end diastolic volume index is 78 ml/m2 (normal range: 65+/-11), the LVEDV is 145 ml (normal range 109+/-23), the LV end systolic volume index is 29 ml/m2 (normal range 18+/-5), the LVESV is 54 ml (normal range 31+/-10), the LV mass index is 40 g/m2 (normal range 67+/-11), and the LV mass is 75 g (normal range 114+/-24). There are no regional wall motion abnormalities present. There is no late gadolinium enhancement to suggest the presence of an underlying fibrosing, infiltrative, or inflammatory process.Left AtriumThe left atrium is normal in size. Right VentricleThe right ventricle is normal in size and systolic function. The overall RV ejection fraction is 56 %, the RV end diastolic volume index is 84 ml/m2 (normal range 69+/-14), the RVEDV is 156 ml (normal range 110+/-24), the RV end systolic volume index is 37 ml/m2 (normal range 22+/-8), and the RVESV is 88 ml (normal range 35+/-13). Right AtriumThe right atrium is normal in size. Aortic ValveThe aortic valve opens widely and there is no significant aortic regurgitation.Mitral ValveThe mitral valve opens widely and there is trace mitral regurgitation.Pulmonic ValveThe pulmonic valve opens widely. There is no significant pulmonic regurgitation.Tricuspid ValveThe tricuspid valve opens widely. There is trace tricuspid regurgitation.AortaThere is a left sided aortic arch with a normal brachiocephalic branching pattern. The aortic root is normal in size.Pulmonary VeinsAll four pulmonary veins drain normally into the left atrium.Pulmonary ArteryThe main pulmonary artery is normal in size. Venous AnatomyThe SVC and IVC are normal in size and drain normally into the right atrium. PericardiumThere is no obvious pericardial disease.Extracardiac FindingsMediastinal lymph nodes are noted. This study is not designed for the specific evaluation of extra-cardiac findings; therefore, the differentiation between artifacts and real extracardiac pathology may be difficult. If clinically indicated, a separate dedicated evaluation should be considered.
1. Normal LV size and systolic function (LVEF 63%) without evidence of underlying myocardial fibrosis, inflammation, or infiltration.2. Normal RV size and systolic function (RVEF 56%).3. See extra-cardiac findings.
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memory impairment No evidence of acute ischemic or hemorrhagic lesion on this scan.Minimal patchy high signal intensities on bilateral periventricular white matters indicate minimal non specific small vessel ischemic disease.The ventricles, sulci and cisterns are symmetric and unremarkable. The gray-white matter differentiation is normal. There is no mass, mass effect, edema, midline shift, intra or extra-axial fluid collection/hemorrhage, or restricted diffusion/acute ischemia. The midline structures and cranial-cervical junction are normal. Normal flow voids are identified in the major intracranial vessels. The paranasal sinuses and mastoid air cells are clear.
Minimal nonspecific small vessel ischemic disease.No evidence of acute ischemic or hemorrhagic lesion on this scan.
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Lung cancer. There is no evidence of intracranial hemorrhage, mass, or acute infarct. There are small areas of encephalomalacia in the right cerebellar hemisphere. There are also mild scattered periventricular and subcortical white matter T2 hyperintensities, which are nonspecific, but compatible with chronic microvascular ischemic disease. There is no abnormal parenchymal or leptomeningeal enhancement. The ventricles and basal cisterns are normal in size and configuration. There is no midline shift or herniation. The major cerebral flow voids are intact. There is mild scattered paranasal sinus mucosal thickening. The orbits, skull, and scalp soft tissues are grossly unremarkable. There is partially-imaged degenerative spondylosis at C4-5.
1. No evidence of metastatic disease.2. Chronic right cerebellar infarcts. I personally reviewed the Images and/or procedure with the Resident/Fellow and agree with this report.
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44-year-old male with new onset seizure. Evaluate for stroke, edema. There is an area of hypodensity in the right frontal subcortical region that may represent edema or encephalomalacia. This could be related to old ischemic change. However, an MRI is recommended for further evaluation. The ventricles and sulci are mildly prominent, which may represent volume loss considering the patient's age. The calvaria and skull base are radiographically normal. The visualized paranasal sinuses and mastoid air cells are normally pneumatized.
Right frontal subcortical hypodensity may represent edema or encephalomalacia. This could be related to old ischemic change. However, an MRI is recommended for further evaluation.
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44-year-old male with shoulder pain. Evaluate for rotator cuff tendinopathy versus partial tear. ROTATOR CUFF: There is perhaps mild thickening and slight increased signal intensity of the insertional fibers of the supraspinatus tendon suggesting mild tendinosis, but we see no fluid-filled tear. The supraspinatus muscle is within normal limits. The infraspinatus tendon and muscle appear intact. The teres minor and subscapularis muscles and tendons appear intact. There is a subchondral cyst within the humeral head which is not necessarily of current clinical significance.SUPRASPINATUS OUTLET: Mild osteoarthritis affects the acromioclavicular joint. There is mild anterior spurring of the acromion process. No fluid is identified within the subacromial subdeltoid bursa.GLENOHUMERAL JOINT AND GLENOID LABRUM: The glenohumeral joint alignment is within normal limits. There is no joint effusion. Given the limitations of a non arthrogram study, the glenoid labrum appears normal. The articular cartilage of the shoulder appears within normal limits.BICEPS TENDON: Given the limitations of a non arthrogram study, the tendon of the long head of the biceps appears within normal limits.
Possible mild supraspinatus tendinosis at its insertion and minimal osteoarthritis of the acromioclavicular joint. We see no rotator cuff tear.
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Right shoulder pain ROTATOR CUFF: The rotator cuff is normal.SUPRASPINATUS OUTLET: The acromioclavicular joint is normal and there is no fluid within the subacromial subdeltoid bursa.GLENOHUMERAL JOINT AND GLENOID LABRUM: The labrum is normal. There are no loose bodies within the joint. The articular cartilage is preserved.BICEPS TENDON: No significant abnormality noted.
Normal appearance of the labrum with no specific findings to account for the patient's shoulder pain.
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34 year old man with non-ischemic cardiomyopathy and palpitations and wide-complex tachycardia. Left VentricleThe left ventricle is normal in size with mildly reduced systolic function. The overall LV ejection fraction is 50%, the LV end diastolic volume index is 103 ml/m2 (normal range: 74+/-15), the LVEDV is 223 ml (normal range 142+/-34), the LV end systolic volume index is 52 ml/m2 (normal range 25+/-9), the LVESV is 112 ml (normal range 47+/-19), the LV mass index is 66 g/m2 (normal range 85+/-15), and the LV mass is 142 g (normal range 164+/-36). There are no regional wall motion abnormalities present. There is no late gadolinium enhancement to suggest the presence of an underlying fibrosing, infiltrative, or inflammatory process. No evidence of myocardial iron overload.Left AtriumThe left atrium is mildly dilated. Right VentricleThe right ventricle is normal in size and systolic function. The overall RV ejection fraction is 52%, the RV end diastolic volume index is 115 ml/m2 (normal range 82+/-16), the RVEDV is 248 ml (normal range 142+/-31), the RV end systolic volume index is 55 ml/m2 (normal range 31+/-9), and the RVESV is 119 ml (normal range 54+/-17).Right AtriumThe right atrium is normal in size.Aortic ValveThe aortic valve opens widely and there is no significant aortic regurgitation.Mitral ValveThe mitral valve opens widely and there is no significant mitral regurgitation.Pulmonic ValveThe pulmonic valve opens widely. There is no significant pulmonic regurgitation.Tricuspid ValveThe tricuspid valve opens widely. There is mild tricuspid regurgitation.AortaThere is a left sided aortic arch with a normal brachiocephalic branching pattern. The aortic root is normal in size.Pulmonary VeinsAll four pulmonary veins drain normally into the left atrium.Pulmonary ArteryThe main pulmonary artery is normal in size.Venous AnatomyThe SVC and IVC are normal in size and drain normally into the right atrium.PericardiumThere is no obvious pericardial disease.Extracardiac FindingsThis study is not designed for the specific evaluation of extra-cardiac findings; therefore, the differentiation between artifacts and real extracardiac pathology may be difficult. If clinically indicated, a separate dedicated evaluation should be considered.
1. Normal LV size with mildly reduced systolic function (LVEF 50%) without evidence of underlying myocardial fibrosis, inflammation, or infiltration.2 Normal RV size and systolic function (RVEF 52%).3. Mild left atrial dilation.
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Male, 53 years old, with history of spastic astrocytoma status post resection in 2012 with increasing headache. Evidence of prior tumor resection from the cerebellum is again seen. The resection cavity is stable in size and morphology. No new signal abnormality is seen. No pathologic enhancement is detected within or adjacent to the cavity. Elsewhere, there is no evidence of significant parenchymal signal abnormality or pathologic enhancement. No edema or mass effect is detected. Ventricular size and morphology are stable and within normal limits. An incidental developmental venous anomaly is evident in the right occipital lobe.
Stable appearance of the cerebellar resection cavity with no evidence to suggest recurrent tumor.
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51-year-old female with right foot pain status post trauma. Assess for anterior process of calcaneus fracture.IMAGE ACQUISITIONS: CT examination of the right foot was performed without IV contrast. Transverse, coronal, and sagittal reformations were performed. Soft tissue and bone windows were reviewed. There is no evidence of fracture. Specifically, the anterior process of the calcaneus appears normal. Mild osteoarthritis affects the first metatarsophalangeal joint. A bipartite medial sesamoid is identified which is a normal variant. Tiny accessory navicular bones are identified which are of doubtful clinical significance.The visualized tendons and ligamentous structures of the ankle appear normal given the limitations of CT relative to MRI. Note is made of a low-lying soleus muscle.Nonspecific subcutaneous edema along the lateral aspect of the foot and ankle.
Mild lateral soft tissue swelling without evidence of fracture.
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Male 26 years old Reason: r/o torn meniscus History: swelling pain MENISCI: There is an obliquely orientated focus of increased signal intensity extending through the peripheral fibers of the posterior horn of the lateral meniscus to the femoral articular surface, indicating a tear that is continuous with the interface of the meniscus with the meniscofemoral ligament. Furthermore the popliteomeniscal fascicles appear distorted and torn. The body and anterior horn of the meniscus demonstrate normal signal intensity and morphology. The medial meniscus demonstrates normal signal intensity and morphology.ARTICULAR CARTILAGE AND BONE: There is edema within the posterior aspect of the lateral tibial plateau as well as the lateral femoral condyle above the anterior horn of the lateral meniscus. The articular cartilage is intact.LIGAMENTS: The anterior cruciate ligament is abnormally thickened and of increased signal intensity indicating at least a partial thickness tear. The slope of the distal fibers is maintained but the proximal fibers are distorted. The posterior cruciate ligament demonstrates normal signal intensity and morphology. EXTENSOR MECHANISM: No significant abnormality noted.ADDITIONAL
Findings consistent with at least a partial-thickness anterior cruciate ligament tear as well as a tear of the posterior horn of the lateral meniscus.
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Female 17 years old Reason: eval for djd; stiff s/p surgery pre-peroneal tendon repair History: ankle pain and stiffness for years TENDONS: No significant abnormality noted.LIGAMENTS: No significant abnormality noted.ARTICULAR SURFACES AND BONE: There is no evidence of DJD or bone compromise. T2 fluid signal on the anterior tibiotalar joint may represent a tibiotalar ganglion. Minimal narrowing of the posterior tibiotalar joint when compared with previous examination. ADDITIONAL
Incidental finding of posterior tibiotalar ganglion and minimal joint narrowing of the posterior tibiotalar joint, otherwise normal examination.
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Adrenal mass seen on CT at outside hospital. ABDOMEN:LIVER, BILIARY TRACT: Status post cholecystectomy. No significant biliary ductal dilatation. No focal liver lesion. The vessels are patent.SPLEEN: No significant abnormality noted.PANCREAS: No significant abnormality noted.ADRENAL GLANDS: 2.0 x 1.4 cm right adrenal lesion demonstrates central T1 and T2-weighted hyperintensity (series 3/23; series 9/43) and a thin peripheral hypointense rim. No loss of signal on out of phase imaging or postcontrast enhancement on the subtraction images.KIDNEYS, URETERS: Atrophic right kidney. Simple left renal cysts. No suspicious renal lesion or hydroureteronephrosis.RETROPERITONEUM, LYMPH NODES: No significant abnormality noted.BOWEL, MESENTERY: No significant abnormality noted.BONES, SOFT TISSUES: Degenerative changes of the spine. Probable benign vertebral body hemangiomas. OTHER: No significant abnormality noted.
The right adrenal lesion measures 2.0 cm, decreased from size reported. In the absence of a known primary the imaging characteristics are most suggestive of adrenal hemorrhage.
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Posterior tibial tendinitis TENDONS: There is a mild amount of fluid surrounding the posterior tibialis, flexor digitorum longus and flexor hallucis longus tendons however the tendons themselves appear normal in caliber and signal. The peroneal tendons and extensor tendons also appear normal.LIGAMENTS: No significant abnormality noted.ARTICULAR SURFACES AND BONE: No significant abnormality noted. Mild osteoarthritis affects the first MTP joint.ADDITIONAL
Perhaps minimal tenosynovitis of the posterior tibialis, flexor digitorum longus, and flexor hallucis longus tendons although the tendons themselves are normal.
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Sarcoidosis, systemic lupus erythematosus, low back pain Five lumbar type vertebral bodies are presumed to be present. Vertebral body heights are within normal limits. Alignment is within normal limits. Bone marrow signal is benign with T1 hyperintense foci scattered within the vertebral bodies compatible with focal fat or hemangiomas. The conus medullaris is normal in position.Mild degenerative changes are seen, as described below:L1-L2: No significant disc disease. No spinal canal or neural foraminal stenosis.L2-L3: No significant disc disease. No spinal canal or neural foraminal stenosis.L3-L4: No significant disc disease. No spinal canal or neural foraminal stenosis.L4-L5: Disc desiccation, mild disc bulge, and dorsal annular fissure. No spinal canal or neural foraminal stenosis. Mild facet arthropathy.L5-S1: Disc desiccation. No spinal canal or neural foraminal stenosis. Moderate facet arthropathy.Paraspinous soft tissues are within normal limits.
Mild degenerative changes in the lumbar spine without significant spinal canal stenosis or neural foraminal stenosis at any level. There is facet arthropathy at L5-S1 bilaterally and to a lesser degree at L4-L5, which may be contributing to patient's low back pain.
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64-year-old male with confusion on Coumadin found down at bedside with no neurologic findings. There is no evidence of intracranial hemorrhage, mass or edema. Diffuse hypodense region within the subcortical and periventricular white matter consistent with small vessel disease, age indeterminate. Well defined hypodense region within the left MCA territory and left cerebellum consistent with previous strokes. No acute cortical stroke is seen, however, if there is clinical concern for acute ischemia, an MRI may be considered. Dense atherosclerotic calcifications noted throughout the large vessels.The ventricles and basal cisterns are normal in size and configuration.The calvaria and skull base are radiographically normal. The visualized paranasal sinuses and mastoid air cells are normally pneumatized.
Small vessel ischemic disease, age indeterminate. If there is clinical concern for acute ischemia, an MRI may be considered.
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Other specified health status [Z78.9], Reason for Study: ^Reason: eval for acute cerebral infarction History: acute on chronic aphasia concerning for stroke There are multifocal restricted diffusion lesions on the left MCA territory including left frontal lobe middle and inferior frontal gyri and left posterior parietal lobe indicating acute to subacute ischemic infarction.Underlying brain shows multifocal patchy FLAIR high signal intensity lesions involving bilateral frontal and parietal lobes (left more than right), as well as right occipital lobe and left temporal lobe with encephalomalacia indicating chronic ischemic infarction.Multifocal scattered FLAIR high signal intensity lesions on bilateral periventricular white matter indicating non specific small vessel ischemic disease.Due to patient motion, gradient-echo sequence was not applied therefore, precise evaluation regarding hemorrhagic lesion is incomplete.The ventricles, sulci and cisterns are symmetric and unremarkable. There is no mass, mass effect, edema, or midline shift. The midline structures and cranial-cervical junction are normal. Normal flow voids are identified in the major intracranial vessels. The mastoid air cells are clear.There is a retention cyst on the right maxillary sinus.Left eye lens signal is not seen indicating prior cataract surgery.
1. Left MCA territorial acute/subacute ischemic infarctions as described above.2. Multifocal bihemispheric chronic ischemic infarctions with encephalomalacia.
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Elevated PSA. PELVIS:PROSTATE:Prostate Size: 5.9 x 6.8 x 8.0 cm.Peripheral Zone: No discrete suspicious focus.Central Gland: Extensive changes of BPH.0.9 x 1.0 cm mid gland medial focus is very low signal intensity on T2-weighted imaging with restricted diffusion (series 1201/19).1.3 x 1.1 cm apex medial focus with low signal intensity on T2-weighted imaging ill-defined margins, restricted diffusion and early arterial enhancement with washout (series 1201/13).1.7 x 0.8 cm apex left lateral focus with ill-defined low signal intensity in T2-weighted sequences and restricted diffusion.Seminal Vesicles: No evidence of seminal vesicle invasion.Extracapsular Extension: No evidence of extracapsular extension.BLADDER: No significant abnormality noted.LYMPH NODES: No significant abnormality noted.BONES, SOFT TISSUES: No significant abnormality noted.OTHER: No significant abnormality noted.
1.Three foci in the transition zone demonstrating low signal intensity in T2-weighted imaging and restricted diffusion may reflect sites of prostatic carcinoma. Alternatively, these may reflect BPH nodules.2.After discussing the findings with the patient the patient agreed to undergo an MR guided biopsy of these lesions.
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83 year-old female history of IPMN. ABDOMEN:LIVER, BILIARY TRACT: Cholelithiasis. No focal hepatic lesions. Mild extra hepatic biliary ductal dilatation with the common bile duct measuring up to 11 mm. No filling defects or masses are present.SPLEEN: No significant abnormality noted.PANCREAS: Unchanged uncinate process cystic lesion measures 1.7 x 1.0 cm (image 32 of series 3). Unchanged body cystic lesion measuring 1.7 x 1.0 cm (image 27 of series 3). Unchanged tail cystic lesion measuring 0.9 x 0.8 cm (image 19 of series 6).ADRENAL GLANDS: No significant abnormality noted.KIDNEYS, URETERS: No significant abnormality noted.RETROPERITONEUM, LYMPH NODES: No significant abnormality noted.BOWEL, MESENTERY: Small gastric diverticulum.BONES, SOFT TISSUES: No significant abnormality noted.OTHER: Postoperative changes of right mastectomy. Ectatic ascending aorta measuring up to 4.3 cm. Trace right pleural effusion.
Stable pancreatic cystic lesions as above.
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Six rule female with history of intracranial METs, now with right-sided headache. There is no evidence of intracranial hemorrhage, mass or edema. Multiple areas of diffuse periventricular and subcortical white matter hypodensity consistent with small vessel ischemic disease, age indeterminate. If there is clinical concern for acute ischemia, an MRI may be considered. Noncontrast evaluation is limited for evaluation of tumor.The ventricles and basal cisterns are normal in size and configuration.The calvaria and skull base are radiographically normal. The visualized paranasal sinuses and mastoid air cells are normally pneumatized.
No acute change.
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Headache, difficulty with potty training and constipation, family history of epilepsy and other diseases of the nervous system, evaluate for syrinx. MRI brain: There is no Chiari malformation. The CSF flow study is technically inadequate. There is no evidence of intracranial hemorrhage, mass, or acute infarct. The brain parenchyma and pituitary gland appear unremarkable. The ventricles and basal cisterns are normal in size and configuration. There is no midline shift or herniation. The major cerebral flow voids are intact. The orbits, skull, paranasal sinuses, and scalp soft tissues are grossly unremarkable.MRI spine: This is a slightly motion degraded exam. The vertebral alignment is within normal limits. The vertebral body and disc space heights are preserved. The vertebral bone marrow signal is unremarkable. There is no significant spinal canal stenosis. The spinal cord displays normal signal and morphology. No evidence of syringohydromyelia. The spinal cord terminates at the upper L1 level. No evidence of fatty filum terminale or intraspinal mass is seen.The paravertebral soft tissues are unremarkable.
1. Unremarkable MRI brain. No evidence of Chiari malformation.2. Unremarkable MRI spine. No evidence of syringohydromyelia.
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Asymptomatic 60 year old woman presents for routine screening mammography. Personal history of benign right breast biopsy in December 2011. Family history of breast cancer in mother, two sisters, maternal cousin, and four paternal cousins. There is scattered fibroglandular tissue in both breasts.Mild parenchymal enhancement is noted bilaterally.Previously described lobulated small mass in the right breast 9:00 position is unchanged, consistent with a benign lesion.No abnormal enhancement is seen in either breast. No abnormal lymph nodes are identified in either axillary region.No abnormal enhancement is seen in either breast. No abnormal lymph nodes are identified in either axillary region.
No MRI evidence for malignancy. BIRADS: 2 - Benign finding.RECOMMENDATION: NS - Routine Screening Mammogram.
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Female 20 years old History: seizure. Some sequences are partially degraded by artifact. There is no evidence of intracranial hemorrhage, mass, or acute infarct. The brain parenchyma appears unremarkable. There is no asymmetry of the hippocampi or evidence of volume loss. There is a nonspecific partially empty sella. The ventricles and basal cisterns are normal in size and configuration. There is no midline shift or herniation. The major cerebral flow voids are intact. The orbits, skull, and scalp soft tissues are grossly unremarkable. Partially visualized mild mucosal thickening of the right maxillary sinus. Evaluation of the paranasal sinuses is limited by artifact.
No specific findings to account for the patient's symptoms. No evidence of intracranial hemorrhage, mass, or acute infarct.
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Clinical question: CVA, TIA, hemorrhage. Signs and symptoms: Aphasia. Nonenhanced head CT:Examination again demonstrates as was noted on prior brain MRI of 24 hours earlier multiple foci of vasogenic edema consistent with multiple intracranial complement the study lesions. The lesion in the basal cistern demonstrate high density and likely representing known hemorrhagic component of tumor. The larger metastatic lesion in the left anterior frontal lobe demonstrates slightly higher than gray matter density also consistent with minimal internal hemorrhage. Mildly high density of vermian metastatic focus is also like lesion sulcal minimal internal hemorrhage.The rest of metastatic foci are evident only by edema without evidence of hemorrhage.There is evidence of regional mass effect at the level of metastatic lesions and without detectable mass effect on the ventricular system or midline shift.
1.Multiple foci of vasogenic edema consistent with patient's known intracranial metastatic lesions not significantly changed since prior exam from 24 hours earlier.2.Several of the lesions demonstrate slight increased density consistent with hemorrhage within the metastatic lesions as was noted on prior MRI.
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75-year-old man status post adrenalectomy for a right adrenal neoplasm. ABDOMEN:LIVER, BILIARY TRACT: Right hepatic lobe calcifications. The liver is otherwise normal in signal and morphology. The patient is status post cholecystectomy. There is no significant intra or extrahepatic duct dilatation.SPLEEN: The spleen is normal.PANCREAS: The pancreas is normal.ADRENAL GLANDS: The patient is status post right adrenalectomy. In the right adrenalectomy bed (series 4, image 29) there is a peripherally T2 hyperintense lesion measuring 22 x 20 mm, previously 17 mm. There is no loss of signal on opposed phase imaging to suggest microscopic fat and this lesion does not significantly enhance until the 3 minute delayed phase of imaging (series 11, image 44). An additional, subcentimeter focus of soft tissue posterior to this lesion appears stable to prior examinations and is most likely postoperative scarring given relative stability.KIDNEYS, URETERS: A left renal cyst is unchanged. The right kidney is normal.RETROPERITONEUM, LYMPH NODES: No significant lymphadenopathy noted.BOWEL, MESENTERY: The partially visualized small bowel and colon are normal.BONES, SOFT TISSUES: No significant abnormality noted.OTHER: No significant abnormality noted.
Enlarging lesion in the right adrenalectomy bed suspicious for residual/recurrent tumor.
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43-year-old female with multiple sclerosis. F/u progression. Again seen are new numerous T2/FLAIR hyperintense lesions predominantly within the supratentorial white matter and including the periaqueductal gray, which appear similar to the previous exam allowing for differences in technique. These lesions are T1 hypointense with some markedly T1 hypointense. There is no evidence of intracranial hemorrhage, mass, midline shift or herniation. The ventricles and basal cisterns are unchanged in size and configuration. The skull and extracranial soft tissues are unremarkable. The major cerebral flow voids are intact. The orbits, skull, paranasal sinuses, and scalp soft tissues are grossly unremarkable.
Allowing for differences in technique, the numerous white matter lesions in the brain compatible with multiple sclerosis are not significantly changed.
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Oligodendroglioma, WHO grade II, pre-treatment planning. There a postoperative findings related to left transfrontal biopsy of an infiltrative T2 hyperintense left insular mass, which measures up to approximately 3 cm. The ventricles and other cerebrospinal fluid spaces are unchanged in size and configuration, including a cystic septum pellucidum and vergae. There is no midline shift or herniation. The major cerebral flow voids are intact. There are skin fiducial markers in position.
Pre-treatment planning MRI for a left insular oligodendroglioma, with skin fiducial markers present.
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42 years, Male, right hemibody numbness. Evaluate for thalamic stroke. No restricted diffusion to suggest acute ischemia. No intracranial hemorrhage. No intracranial mass or mass-effect. The ventricles are within normal limits in size and configuration. Minimal scattered foci of T2/FLAIR hyperintensity are seen in the bilateral subcortical and periventricular white matter, which are nonspecific. There is no significant parenchymal signal abnormality. Apparent T2 hyperintensity involving the medulla is likely artifactual and demonstrates no corresponding signal abnormality on the FLAIR or diffusion sequences. Brain parenchyma is otherwise unremarkable for age. Major flow-voids are preserved. Sella and orbits are grossly within normal limits. Paranasal sinuses and mastoid cells are clear. Bone marrow signal and extracranial soft tissues are within normal limits.
Brain parenchyma appears within normal limits for age. Specifically, no evidence of thalamic infarct.
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Male, 24 years old, multiple sclerosis. Recently diagnosed with MS, on October 2016 and has follow up with Dr Ciprianni at U of C. He was recently started on Tecfidera about 2 weeks ago. Over the last week he reports to be feeling progressive numbness on L hand and L toes. He was referred for admission for MS flare and treatment with IV steroids. Multiple imaging series are degraded by patient motion. Small T2/STIR hyperintense lesions are partially visualized on sagittal imaging in the right middle cerebellar peduncle and left cerebellar hemisphere white matter, which were better visualized on the outside brain MR examination. There are two small peripherally located foci of T2/STIR signal abnormality on the right at the C2 and C2-3 levels. The C2-3 level lesion may be new. A larger T2/STIR signal lesion in the spinal cord is present on the left from lower C4 level to the mid C6 level, which appears to be new. There is moderate associated expansion of the spinal cord at the C5 level. There is also enhancement of the lesion at the C4-C5 to the C5-C6 levels within the left and dorsal aspects of the spinal cord, suggesting active demyelination.There is normal alignment of the cervical spine, with normal cervical lordosis. Vertebral body and intervertebral disc heights are maintained. There is no significant disc bulge or herniation. No high-grade foraminal stenosis in the cervical spine, within the limitations of motion degradation. THORACIC SPINE
1. Interval progression of demyelinating disease in the cervical cord with a new lesion extending from the C4-C5 to C5-C6 levels involving the left and dorsal aspects of the cervical spinal cord. There is associated enhancement consistent with active demyelination.2. No abnormal signal identified in the thoracic spinal cord.3. Partially visualized demyelinating lesions within the left cerebellar hemisphere and right middle cerebellar peduncle, better visualized on outside MRI of the brain.
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Status post liver transplant. Known seroma with inflammation in the region of the left brachial plexus.Additional clinical history from electronic medical records: 63-year-old female with left upper extremity numbness, tingling and weakness. History of orthostatic liver transplant status on 10/5/2015 for hepatitis C/EtOH related cirrhosis with HCC. Diagnosed with CRPS type II of LUE status post liver transplant where her L arm was injured during surgery (swollen 2-3 x normal size). Had L stellate ganglion block in Marc 2016 but with only brief improvement. The surgical incision is again seen along the left upper chest. The underlying T2-hyperintensity in the left pectoris major and minor muscles remains unchanged as well as the mild distortion, probably scarring. The tiny subpectoral collection demonstrates less T2-hyperintensty and is smaller, probably a resolving seroma/hematoma. The adjacent left subclavian vein still shows slight distortion and suggestion of narrowing adjacent to a surgical clip, though looks patent upstream and downstream from this point. There is no asymmetric signal abnormality involving the left brachial plexus. There is no mass along its course but the above-described scarring findings are in the vicinity of the divisions/cords of the plexus. There are small left pectoral lymph nodes.Multilevel degenerative cervical spine disease is not significantly changed since the previous examination, most pronounced at C6-C7 where a disc extrusion with cranial migration is present minimally indenting the left ventrolateral aspect of the spinal cord. Please refer to the report of the previous cervical spine MRI from November 30, 2015 for full details.
1.There is scarring related to the previous left upper chest incision, involving the underlying muscles. There is suggestion of underlying focal stenosis/tethering of the left subclavian vein just adjacent to a surgical clip. Patency of the vein is probably better assessed by Doppler ultrasound, if clinically warranted.2.As discussed previously, though there is no definite injury to the left brachial plexus, the plexus passes reasonably close to the subclavian vein operative field where there is evidence of some scarring and tethering which may have affected the divisions/cords of the plexus. 3.The previously described small subpectoral seroma or hematoma has further regressed.
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Metastatic melanoma on Temodar. The intrinsically T1 hyperintense lesions in the bilateral cerebral hemispheres are stable to slightly decreased in size. For example, a lesion in the left occipital lobe measures 4 mm in diameter, previously also 4 mm, while a lesion in the right anterior cingulate gyrus measures 3 mm in diameter, previously 5 mm. There is no appreciable vasogenic edema associated with the lesions. There is no evidence of intracranial hemorrhage or acute infarct. The ventricles and basal cisterns are unchanged in size and configuration. There is no midline shift or herniation. The major cerebral flow voids are intact. The orbits, skull, paranasal sinuses, and scalp soft tissues are grossly unremarkable.
Stable to slight interval decrease in size of the brain metastases.
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48-year-old male with history of lumbar cracking and popping with movement Anterior vertebral body osteophytes along the lower lumbar spine with mild L4-L5 and L5-S1 disk space narrowing. Vertebral body heights are maintained. Alignment is within normal limits on flexion and extension views.
Degenerative disk disease as described above.
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51-year-old male with acute psychosis, history of pituitary adenoma There is redemonstration of a large sellar lesion measuring 4.1 x 3.3 x 2.2 cm in sagittal and coronal planes (sagittal image 28, coronal image 32). While the size of the sellar lesion is similar to 2004, the mass appears heterogeneously hypodense on CT which is surprising based on prior MRI appearance which was more solid appearing. This may suggest interval treatment. As before, there is remodeling of the sella by the mass, with distortion of the posterior walls of the sphenoid sinus. Relationship to the chiasm is poorly defined based on this CT.There is no acute intracranial hemorrhage with special attention to the abnormal sella turcica. There is also no focal fluid collection. Ventricles and sulci retain normal size/configuration.Gray-white matter differentiation is preserved. There is no focal parenchymal lesion or mass. There is no midline shift or basal cistern effacement.Unremarkable visualized portions of the orbits. Paranasal sinuses are clear to the extent visualized. Mastoid air cells are also clear. Probable small quantities of cerumen in the external auditory canals.
1.No acute intracranial abnormality. Specifically no acute intracranial hemorrhage or generalized mass effect.2.Redemonstration of remodeled sella consistent with previously seen pituitary adenoma. The contents of the sella are now predominately hypodense which raises possibility of interval treatment. MRI would be required to evaluate extent of remaining tumor and to define relationship to surrounding structures.
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59 year old with breast pain. Breast parenchyma is almost entirely fat in both breasts.Minimal parenchymal enhancement is noted bilaterally.No abnormal enhancement is seen in either breast. No abnormal lymph nodes are identified in either axillary region.
No MRI evidence for malignancy. BIRADS: 1 - Negative.RECOMMENDATION: NS - Routine Screening Mammogram.
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Female 44 years old with right knee pain. MENISCI: The medial and lateral menisci are intact.ARTICULAR CARTILAGE AND BONE: There is thinning of the cartilage along the medial facet and median ridge of the patella and trochlea. There is a 3 mm full thickness cartilage defect along the median ridge of the patella with an associated subchondral cyst. The articular cartilage of the femoral condyles and tibial plateau is otherwise within normal limits.LIGAMENTS: The anterior cruciate ligament, posterior cruciate ligament, medial collateral ligament, and lateral collateral ligament complex are intact. EXTENSOR MECHANISM: The extensor mechanism is intact.ADDITIONAL
Mild chondromalacia patella.
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Female, 90 years old, with left gluteal and leg pain, worse at the posterior coccyx. A mild levocurvature of lumbar spine may be positional. Sagittal alignment is unremarkable. Vertebral body heights are preserved. Mild endplate edema is seen along the superior L2 endplate. Fatty degenerative endplate signal change is noted at L3-4 and L4-5.The visualized distal spinal cord, conus and nerve roots of the cauda equina are unremarkable except as discussed below.L1-2: Minimal disc bulging. No significant spinal canal or foraminal stenosis. L2-3: Minimal disc bulging. Small right foraminal protrusion. No significant spinal canal or foraminal stenosis L3-4: Mild facet arthropathy and ligamentum flavum thickening. Bulging disc asymmetric to the right. Narrowing of the right lateral recess but no significant generalized spinal canal stenosis. Moderate right foraminal narrowing. L4-5: Moderate facet arthropathy and ligament thickening. Bulging disc. Moderate generalized spinal canal narrowing with some crowding of the cauda equina. Severe right and mild left foraminal narrowing. L5-S1: Facet arthropathy. Central and left paracentral disc protrusion. The left lateral recess is significantly narrowed, though there is no generalized spinal canal stenosis. Severe left foraminal narrowing.
Multilevel disc degeneration is seen. Most notably, at L3-4 there is a moderate generalized spinal canal stenosis and severe right foraminal narrowing; and at L5-S1, there is significant narrowing of the left lateral recess and severe left foraminal narrowing.
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Metastatic renal cell carcinoma with growing destructive lesion at L1. Five lumbar type vertebral bodies are presumed to be present. Vertebral body heights are within normal limits. Alignment is within normal limits. There is anenhancing T1 hypointense 2.5 x 1.4 cm mass centered within the left L1-L2 neural foramen and compressing the left L1 nerve root. There is caudal epidural extension. There is loss of the adjacent L1 vertebral body cortex. There are few foci of T1 and T2 hyperintensity within the lumbar vertebral bodies, probably hemangiomas. The conus medullaris is normal in position.The sacrum and bilateral iliac bones are heterogeneous on T1, with suppression on fat saturation, probably fatty infiltration. There is disc desiccation at L5-S1 with a disc bulge and right para median-central annular fissure. The disc bulge minimally abuts the left L5 nerve root. Paraspinous soft tissues are within normal limits.
Enhancing mass centered within the left L1-2 foramen, with disruption of the vertebral body cortex and extension into the epidural space, probable renal metastasis.
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13-year-old female with pain and mechanical symptoms in the left knee. MENISCI: The medial and lateral menisci are normal.ARTICULAR CARTILAGE AND BONE: Generalized thinning of the patellar cartilage is noted without focal defects. The articular cartilage within the lateral and medial tibiofemoral compartments is unremarkable. No bone marrow edema.LIGAMENTS: The cruciate and collateral ligaments are intact. EXTENSOR MECHANISM: The extensor mechanism is intact.ADDITIONAL
1.Generalized thinning of the patellar cartilage without focal defects. Findings may represent chondromalacia patella.2.No evidence of meniscal or ligamentous injury.
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Ms. Faith is a 50 year old female with recently diagnosed right breast malignancy. She presents for MRI for further evaluation. There is heterogeneous amount of fibroglandular tissue in both breasts. Marked background parenchymal enhancement is noted bilaterally, which limits the sensitivity of this examination.In the right upper outer breast, there is an irregular enhancing lesion identified measuring 2.0 x 1.4 x 2.2 cm (AP x ML x SI). Susceptibility artifact from biopsy marker clip is seen centrally within this lesion, compatible with biopsy proven malignancy. There is no additional abnormal enhancement present in the right breast. There is no abnormal enhancement present in the left breast. Of note, there are several non-dilated, non-enhancing retroareolar ducts with fluid identified in the left breast. No abnormal axillary lymph nodes are identified in either axillary region.
(1) Unifocal malignancy of the right breast, measuring up to 2.2 cm. Clip is in appropriate position. If breast conservation therapy is desired, the clip can be used as targeting for preoperative surgical guidance. (2) No MRI evidence for malignancy in the left breast. BIRADS: 6 - Known cancer.RECOMMENDATION: X - No Letter.
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Diagnosis: Other malaise and fatigueClinical question: Please evaluate for focal abnormality particularly thalamusSigns and Symptoms: Episode of transient left face, arm, and leg weakness with painComments: Please obtain without sedation if possible | The CSF spaces are appropriate for the patient's stated age with no midline shift. No abnormal enhancing mass lesions are appreciated intracranially. No intracranial hemorrhage is identified. No edema is identified within the brain parenchyma.Normal vascular flow voids are present in the distal carotid and vertebral arteries, the basilar artery and the proximal anterior, middle and posterior cerebral arteries as well as the internal cerebral veins and superior sagittal sinus.The visualized portions of the paranasal sinuses are clear. The visualized portions of the mastoid air cells are clear. The visualized portions of the orbits are intact.
MRI of the brain is within normal limits
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History of Crohn's disease. Evaluate for evidence of active inflammation. ABDOMEN:LIVER, BILIARY TRACT: No significant abnormality noted.SPLEEN: No significant abnormality noted.PANCREAS: No significant abnormality noted.ADRENAL GLANDS: No significant abnormality noted.KIDNEYS, URETERS: No significant abnormality noted.RETROPERITONEUM, LYMPH NODES: No significant abnormality noted.BOWEL, MESENTERY: The small bowel is adequately distended with oral contrast. The small bowel fold pattern is maintained. The terminal ileum is well seen and demonstrates no significant active inflammation. There are intermittent regions of jejunal underdistention likely related to peristalsis without specific evidence of active inflammation. No flow-limiting stricture.The descending colon is featureless. Starting at the splenic flexure the colon demonstrates mild to moderate regions of long-segment mild T2-weighted hyperintensity, restricted diffusion and post-contrast enhancement compatible with active inflammation. This is most severe at the sigmoid colon. At the level of the rectosigmoid is a short segment skip region with subsequent short segment skip lesion. The distal rectum appears spared. Proximal to the splenic flexure I suspect regions of intermittent peristaltic contraction (see dynamic images) but no flow-limiting stricture or definite evidence of active inflammation. There is engorgement of the pericolonic vasa recta and scattered small reactive lymph nodes. There is no significant upstream dilatation to suggest a flow-limiting stricture.No evidence of sinus tract or fistula formation. No free fluid or loculated fluid collection.BONES, SOFT TISSUES: No significant abnormality noted.OTHER: No significant abnormality noted.PELVIS:UTERUS, ADNEXA: No significant abnormality noted.BLADDER: No significant abnormality noted.LYMPH NODES: No significant abnormality noted.BOWEL, MESENTERY: The descending colon is featureless. Starting at the splenic flexure the colon demonstrates mild to moderate regions of long-segment mild T2-weighted hyperintensity, restricted diffusion and post-contrast enhancement compatible with active inflammation. This is most severe at the sigmoid colon. At the level of the rectosigmoid is a short segment skip region with subsequent short segment skip lesion. The distal rectum appears spared. Proximal to the splenic flexure I suspect regions of intermittent peristaltic contraction but no flow-limiting stricture or definite evidence of active inflammation. There is engorgement of the pericolonic vasa recta and scattered small reactive lymph nodes. There is no significant upstream dilatation to suggest a flow-limiting stricture.BONES, SOFT TISSUES: No significant abnormality noted.OTHER: No significant abnormality noted.
No significant active inflammation of the small bowel. Moderate active inflammation of a featureless distal colon from the splenic flexure extending distally with short skip areas near the rectosigmoid and distal rectum. The inflammation is most severe of the sigmoid colon. No flow-limiting stricture or evidence of sinus tract/fistula formation.
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Evaluate progress of left subdural hemorrhage, assess left quadrigeminal cistern plate lipoma, calcifications: left subdural hemorrhage, lipoma, calcifications. There is a low T2 and high T1 signal subdural hematoma along the left posterior falx cerebri that measures up to 5 mm in thickness, which is not significantly changed. There is also perhaps a trace subdural hematoma along the right aspect of the posterior falx cerebri. There is lipoma within the left quadrigeminal plate cistern, which measures up to 8 mm. There is a low T2 and high T1 signal right scalp hematoma that measures up to 10 mm in thickness and a similarly low T2 and high T1 signal right scalp hematoma that measures up to 10 mm in thickness, both of which are confined by the sutures. There is no evidence of intracranial mass or acute infarct. There is no discernible abnormal intraparenchymal susceptibility effect. The degree of sulcation and myelination is likely related to prematurity. The ventricles are unchanged, accounting for differences in technique. There is no midline shift or herniation. The major cerebral flow voids are intact.
1. Unchanged small subdural hematoma along the left posterior falx cerebri and perhaps trace subdural hemorrhage along the right falx cerebri.2. Unchanged bilateral cephalohematomas, right larger than left, and superimposed caput succedaneum. 3. Small left quadrigeminal plate cistern lipoma.4. No discernible brain parenchymal calcification or hemorrhage.
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Pain in right hip [M25.551], Reason for Study: ^Reason: sciatica type pain - pt previously on long term steroids History: see above For the purpose of this dictation, the lowest visualized intervertebral disc space is labeled L5-S1. There is normal lumbar lordosis. The spine alignment is anatomic. The vertebral body height is preserved. The bone marrow and end plates demonstrate a normal MR appearance. The signal of the visualized cord is normal. The conus medullaris terminates at the T12-L1 level. There is no evidence of abnormal enhancement, cord compression or mass. Degenerative changes are specified by the intervertebral level as follows: T12-L1: no neuroforaminal narrowing or spinal stenosis. L1-L2: no neuroforaminal narrowing or spinal stenosis. L2-L3: Diffuse bulging of disc with ligamentum flavum thickening, resulting minimal spinal canal stenosis. No neuroforaminal narrowing. L3-L4: no neuroforaminal narrowing or spinal stenosis. L4-L5: Disc desiccation. There is focal disc bulging toward left side lateral recess which narrows left side neural foramen. L5-S1: no neuroforaminal narrowing or spinal stenosis.
1. Broad-based focal disc bulging toward left side neural foramen of L4-5.2. Minimal spinal canal stenosis at the level of L23.
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There is a hypoenhancing lesion in the right aspect of the pituitary gland that again measures up to 7 x 7 x 5 mm (AP x TV x CC). No evidence of macroadenoma. Infundibulum is midline. There is no suprasellar extension, mass effect upon the optic apparatus, or abnormality involving the cavernous sinuses. The carotid artery flow voids are intact.
Unchanged 7 mm pituitary microadenoma.