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Archives of Pathology & Laboratory Medicine | 2001

Renal angiomyolipoma: further immunophenotypic characterization of an expanding morphologic spectrum.

Chad H. Stone; Min W. Lee; Mahul B. Amin; Hadi Yaziji; Allen M. Gown; Jae Y. Ro; Bernard Têtu; Francois Paraf; Richard J. Zarbo

BACKGROUNDnRenal angiomyolipoma is a benign tumor histologically characterized by proliferation of spindle cells, epithelioid cells, and adipocytic cells in concert with many thick-walled blood vessels. To add further diagnostic confusion, an epithelioid cell-predominant variant of renal angiomyolipoma has recently been described. HMB-45 immunoreactivity correlates with ultrastructural striated organelles that closely resemble premelanosomes, although no evidence of melanogenesis has been documented in this tumor.nnnOBJECTIVEnTo further characterize the immunophenotypic and ultrastructural profile of renal angiomyolipoma based on phenotypic cell type (epithelioid, spindle, and adipocytic cell).nnnDESIGNnFormalin-fixed, paraffin-embedded tissues from 27 renal angiomyolipomas and 8 renal cell carcinomas were immunostained with monoclonal antibodies to the melanoma-associated antigens HMB-45, HMB-50, NKI/C3 (CD63), and tyrosinase; the smooth muscle-related antigens calponin and muscle-specific actin (HHF-35); S100; and cytokeratin (CK). All renal angiomyolipomas were also immunostained with a polyclonal antibody to renin. Ultrastructural examination was performed on 9 selected cases.nnnRESULTSnAll renal angiomyolipomas stained positive for HMB-45, HMB-50, NKI/C3, muscle-specific actin (HHF-35), and calponin. Overall, HMB-45, HMB-50, and NKI/C3 preferentially stained the epithelioid cells. Tyrosinase staining was present in 50% of the renal angiomyolipomas with adequate tissue for staining (12 of 24 cases); positive staining and intensity paralleled HMB-45, HMB-50, and NKI/C3. Muscle-specific actin (HHF-35) and calponin preferentially stained the spindle cells. The adipocytic cells stained positive for both melanoma-associated antigens and smooth muscle antigens. Epithelioid cells, spindle cells, and adipocytic cells were CK, S100, and renin negative. Ultrastructural findings paralleled immunohistochemical staining patterns. Premelanosome-like organelles and electron dense granules were more readily detected in the epithelioid cells within the tumor, whereas ultrastructural characteristics of smooth muscle cells were more easily found in the spindle cells. All renal cell carcinomas stained positive for CK, NKI/C3 staining was variable, and all were negative for HMB-45, HMB-50, smooth muscle actin (HHF-35), and calponin.nnnCONCLUSIONnIn renal angiomyolipoma, the epithelioid and spindle cells have preferential staining patterns for melanoma-associated antigens versus smooth muscle antigens, respectively. Positivity in renal angiomyolipoma for HMB-50, NKI/C3, and tyrosinase, in addition to HMB-45, provides evidence for the presence of different melanoma-associated gene products. Immunophenotypic overlap of the 3 histologically distinct renal angiomyolipoma cell populations suggests a common cell line, supporting a unitarian concept for renal angiomyolipoma. Ultrastructural characteristics of the 3 renal angiomyolipoma cell phenotypes parallel the immunophenotype, giving further support to a common cell line. Our study lends further credence to the perivascular epithelioid cell concept as proposed by Bonetti and colleagues.


Advances in Anatomic Pathology | 1997

Collecting duct carcinoma of the kidney

Mahul B. Amin; Murali D. Varma; Satish K. Tickoo; Jae Y. Ro

Collecting duct carcinoma is a distinctive hislologic subtype of renal cell carcinoma which has recently gained acceptance as a clinicopathologic entity. Approximately 50 cases have been described, with the largest series to date reports 12 cases. Based on the literature experience certain key characteristics regarding this tumor emerge, including predilection for younger age, epicenter in renal medulla, high grade nuclear features with desmoplasia and mucin production, and aggressive clinical course. Origin from the collecting duct is based on the observation of dysplastic changes in the adjacent collecting ducts as well as immunohistoehemical reactivity for Ulex europaeus agglutinin-1 lectin, peanut lectin agglutinin and high molecular weight cytokeratin. Recently there is evidence that the histologic spectrum of collecting duct carcinoma may be wider than that published. In this article we review the clinical and pathologic features of collecting duct carcinoma based on the reported cases and place them into perspective with the putative widening histologic spectrum.


The American Journal of Surgical Pathology | 1998

Histologic variations in the epididymis: Findings in 167 orchiectomy specimens

Varsha I. Shah; Jae Y. Ro; Mahul B. Amin; Seema Mullick; Tipu Nazeer; Alberto G. Ayala

Nonpathologic morphologic variations in the epididymal histology in 167 orchiectomy specimens were analyzed to assess and document the nature, frequency, and possible relation to patient age and underlying testicular pathology. Variations in histology included intranuclear eosinophilic inclusions, lipofuscin pigment, cribriform hyperplasia, Paneth cell-like metaplasia, and nuclear atypia. Intranuclear eosinophilic inclusions were observed in 72.5% of patients, and they appeared to occur at an older age than cribriform hyperplasia and Paneth cell-like metaplasia. Lipofuscin pigment was found in 32.9% of patients; this change was observed predominantly in ductuli efferentes and was more commonly associated with obstructive changes. Cribriform hyperplasia was seen in 41.9% of patients, and it occurred in 1 normal testis and in 33 testes with diverse pathologic alterations. Paneth cell-like metaplasia characterized by bright eosinophilic intracytoplasmic hyaline-like granules and globules, was present in 8.3% of patients and was accompanied by changes of obstruction in almost all instances. The globules were strongly periodic acid-Schiff positive, both before and after diastase digestion, and were negative for chromogranin A, KP-1, and MAC387 immunostains. Nuclear atypia, similar to that seen in seminal vesicles, was focally present in 13.8% of patients and tended to occur at an older age. The authors conclude that variations in epididymal morphology are fairly common and, therefore, surgical pathologists should be aware of these changes. Although exuberant in some patients, in no cases did these variations cause serious diagnostic problems.


Modern Pathology | 1997

Histologic variants of adenocarcinoma and other carcinomas of prostate: pathologic criteria and clinical significance.

Todd L. Randolph; Mahul B. Amin; Jae Y. Ro; Alberto G. Ayala


American Journal of Clinical Pathology | 1998

Discriminant Nuclear Features of Renal Oncocytoma and Chromophobe Renal Cell Carcinoma: Analysis of Their Potential Utility in the Differential Diagnosis

Satish K. Tickoo; Mahul B. Amin


Modern Pathology | 1999

Effect of formalin fixation and epitope retrieval techniques on antibody 34betaE12 immunostaining of prostatic tissues.

Varma M; Linden; Mahul B. Amin


Modern Pathology | 1993

Immunohistologic characterization of gastrointestinal stromal tumors: a study of 82 cases compared with 11 cases of leiomyomas.

Ma Ck; Mahul B. Amin; Kintanar E; Linden; Richard J. Zarbo


American Journal of Clinical Pathology | 1993

Fine-Needle Aspiration Cytologic Study of Myofibroblastoma of the Breast: Immunohistochemical and Ultrastructural Findings

Mahul B. Amin; Cary A. Gottlieb; Maryann Fitzmaurice; Arthur R. Gaba; Min W. Lee; Richard J. Zarbo


American Journal of Clinical Pathology | 1997

Small intestinal stromal tumors: a clinicopathologic study of 20 cases with immunohistochemical assessment of cell differentiation and the prognostic role of proliferation antigens.

Chan K. Ma; Mariza N. De Peralta; Mahul B. Amin; Michael D. Linden; Alexander A. Dekovich; James J. Kubus; Richard J. Zarbo


Archives of Pathology & Laboratory Medicine | 1993

Computerized static DNA ploidy analysis of prostatic intraepithelial neoplasia

Mahul B. Amin; Daniel Schultz; Richard J. Zarbo; Kubus J; Shaheen C

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Min W. Lee

Henry Ford Health System

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Allen M. Gown

University of Washington

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Chan K. Ma

Henry Ford Health System

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Hadi Yaziji

University of Texas MD Anderson Cancer Center

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