R. Nagarjun Rao
Medical College of Wisconsin
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Archives of Pathology & Laboratory Medicine | 2002
Vinod B. Shidham; Mamatha Chivukula; Dilip Gupta; R. Nagarjun Rao; Richard A. Komorowski
CONTEXT The differential diagnosis of gastrointestinal stromal tumors (GIST) and solitary fibrous tumors (SFT) may be a diagnostic challenging because of overlapping clinicopathologic features. Many studies have shown consistent immunoreactivity for CD117 (c-Kit) in GIST. However, only a few studies have evaluated CD117 expression in SFT, and these studies have used an antibody from Santa Cruz Biotechnology. In non-GIST lesions, reactivity with this antibody has been shown to differ from that with a CD117 antibody from Dako Corporation. The immunoreactivity of SFT with the Dako CD117 antibody has not been reported. Conversely, CD99 is a marker for SFT, and its expression in GIST has not been evaluated. OBJECTIVE To study the immunohistochemical profiles of GIST and SFT to evaluate their diagnostic overlap. DESIGN We studied the immunoreactivity of 27 unequivocal GIST and 19 unequivocal extra-abdominal SFT for CD117, CD34, CD99, alpha-smooth muscle actin, vimentin, CD31, S100 protein, and muscle-specific actin. All antibodies, including CD117, were from Dako Corporation. RESULTS We found positive immunoreactivity for CD117 in 100% of GIST and none of SFT; for CD34 in 89% of GIST, and 100% of SFT; for CD99 in 89% of GIST and 100% of SFT; for alpha-smooth muscle actin in 48% of GIST and 31% of SFT; for vimentin in 89% of GIST and 90% of SFT; and for muscle-specific actin in 22% of GIST and none of SFT. None of the GIST or SFT showed immunoreactivity for CD31 and S100 protein. CONCLUSIONS The major difference between GIST and SFT was strong CD117 immunoexpression in all GIST and an absence of this expression in all SFT. With the exception of muscle-specific actin, the prevalence of immunoreactivity for the markers studied did not differ substantially between these 2 tumors. We conclude that GIST and SFT show distinctly divergent immunoprofiles with respect to CD117 and muscle-specific actin.
Leukemia & Lymphoma | 2004
Bal Kampalath; Nashwa Abed; Christopher R. Chitambar; Peter vanTuinen; Gargi Chakrabarty; Gerald Hanson; R. Nagarjun Rao; Vinod B. Shidham; Chung-Che Chang
We report a rare case of small cell carcinoma (SCC) of lung, metastatic to ipsilateral hilar and peribronchial lymph nodes with synchronous mantle cell lymphoma (MCL), in a 58-year-old female. She was treated with Cisplatin, Etoposide, and Rituximab, and remained in complete remission for approximately two and a half years following the initial diagnosis. To the best of our knowledge, synchronous SCC and MCL or SCC metastatic to lymph nodes involved by MCL has not been previously reported. In this case, the features of MCL were very inconspicuous in the lymph nodes with extensive metastases of SCC. The presence of MCL was confirmed by immunohistochemistry and fluorescence in situ hybridization (FISH). The co-existence of lymphoma and metastatic carcinoma in the same lymph node, as seen in this case, highlights the significance of analyzing subtle lymphoid architectural changes, and applying ancillary studies such as immunohistochemistry and molecular analysis in suspicious cases. The management of synchronous SCC and MCL requires consideration of their respective biologic behavior, and cumulative toxicity of treatment regimens of both tumors. In such cases an optimum treatment strategy should be adopted to cover both malignancies with minimal toxic effect.
BMC Musculoskeletal Disorders | 2003
Vinod B. Shidham; Ashwini Chavan; R. Nagarjun Rao; Richard A. Komorowski; Zeenath Asma
BackgroundInterpretation of small biopsy fragments from suspected lesions of fibrous dysplasia with unusual clinical and / or radiological features may be challenging due to wide histomorphological spectrum of stromal appearances. Awareness of these variations should improve diagnostic confidence.MethodsWe retrospectively studied 26 cases of fibrous dysplasia (F- 19, M- 7; Ages ranged from 10 to 53 years) with confirmed diagnosis. The sites of the lesions were skull bones (9), humerus (1), femur (8), tibia (2), fibula (3), talus (1), mandible (1), and maxilla (1).ResultsDifferent stromal patterns, variably admixed with the classical pattern, were observed in 58%(15/26) of the cases. 20%(3/15) of these had more than one pattern. Focal fatty metamorphosis as groups of fat cells in the central portion of the lesion in the stroma of fibrous dysplasia between osseous trabeculae was observed in 23%(6/26) cases. Other patterns included myxoid stroma in 16%(4/26), collagenization of stroma in 12%(3/26), stroma rich pattern (with paucity of trabeculae) in 12%(3/26), foci of few foam cells in 23% (6/26), and calcified spherules in 12%(3/26). Focal osteoblastic rimming of trabeculae was observed only in 4%(1/26).ConclusionsVarious stromal variations and previously unreported fatty metamorphosis were frequently observed in fibrous dysplasia.
American Journal of Clinical Pathology | 2002
Vinod B. Shidham; Zeenat Asma; R. Nagarjun Rao; Ashwini Chavan; Jinobya Machhi; Urias Almagro; Richard A. Komorowski
Diagnostic Cytopathology | 2003
Vinod B. Shidham; Chung-Che Chang; R. Nagarjun Rao; Richard A. Komorowski; Mamatha Chivukula
BMC Cancer | 2003
Vinod B. Shidham; Dan Qi; R. Nagarjun Rao; Scott Acker; Chung-Che Chang; Bal Kampalath; Glen Dawson; Jinobya Machhi; Richard A. Komorowski
Archives of Pathology & Laboratory Medicine | 2005
R. Nagarjun Rao; Chung-Che Chang; Nevin Uysal; Kenneth Presberg; Vinod B. Shidham; Joseph F. Tomashefski
Diagnostic Cytopathology | 2002
Mamatha Chivukula; Raj D. Rao; Janobya Macchi; Farrukh Ghazala; R. Nagarjun Rao; Richard A. Komorowski; Vinod B. Shidham
BMC Clinical Pathology | 2007
Vinod B. Shidham; Ashwini W Pandit; R. Nagarjun Rao; Zainab Basir; Anjani Shidham
Diagnostic Cytopathology | 2004
Vinod B. Shidham; R. Nagarjun Rao; Jinobya Machhi; Ashwini Chavan