Expression of Müllerian Inhibiting Substance, CD99 and HEA125 in Ovarian Tumors

F. Kommoss; E. Oliva; R. H. Young; F. Bittinger; C. J. Kirkpatrick; D. Schmidt

doi:10.1055/s-2001-14147

Geburtshilfe und Frauenheilkunde, Table of Contents

Geburtshilfe Frauenheilkd 2001; 61(5): 274-279
DOI: 10.1055/s-2001-14147

Original Article

Georg Thieme Verlag Stuttgart · New York

Expression of Müllerian Inhibiting Substance, CD99 and HEA125 in Ovarian Tumors

Zur Expression von Müller-Gänge inhibierendem Hormon, CD99 und HEA125 in OvarialtumorenF. Kommoss¹ , E. Oliva² , R. H. Young² , F. Bittinger³ , C. J. Kirkpatrick³ , D. Schmidt¹

¹ Institut für Pathologie, Referenzzentrum für Gynäkopathologie, Mannheim
² Department of Pathology, Massachusetts General Hospital, Harvard Medical School, Boston, USA
³ Institut für Pathologie, Universitätskliniken Mainz, Mainz

Abstract

Summary

Objective

The expression of Müllerian inhibiting substance (MIS), CD99 (MIC-2 gene product), and HEA125 in ovarian tumors is potentially useful for diagnostic purposes.

Methods

We studied the expression of MIS, CD99, and an epithelial cell-associated antigen recognized by antibody HEA125 in a series of 179 ovarian tumors using monoclonal or polyclonal antibodies and standard immunohistochemical techniques.

Results

MIS was consistently detected in primary and metastatic sex cord tumors with annular tubules (SCTAT) (n = 9). 3 of 9 adult granulosa cell tumors (AGCT), 4 of 8 juvenile granulosa cell tumors (JGCT), 3 of 9 Sertoli cell tumors (SCT), 2 of 2 unclassified sex cord tumors, 2 of 7 steroid cell tumors, 1 of 1 gonadoblastoma (sex cord cells positive, germ cells negative), 3 of 8 female adnexal tumors of probable wolffian origin (FATPWO), and 2 of 4 small cell carcinomas of the hypercalcemic type (SCCHCT) were also MIS positive. In contrast, 9 thecomas, 10 fibromas, 10 fibrosarcomas, 8 sclerosing stromal tumors (SST), and 6 Sertoli-Leydig cell tumors (SLCT) were MIS negative. All 11 primary and metastatic JGCT were CD99 positive. In addition, 4 of 13 AGCTs, 3 of 11 thecomas, 3 of 11 SSTs, 3 of 11 SCTs, 2 of 10 SLCTs, 2 of 12 SCTATs, 1 of 1 gynandroblastoma, 1 of 2 unclassified sex cord tumors, and 4 of 12 SCCHCTs were also CD99 positive. However, 11 fibromas, 10 fibrosarcomas, 9 steroid cell tumors, 5 gonadoblastomas, and 10 FATPWOs were CD99 negative. Likewise, except for weak focal CD99 immunostaining in 1 of 3 yolk sac tumors (YST), all 16 remaining germ cell tumors and all 18 borderline or malignant epithelial-stromal tumors were negative. HEA125 immunoreactivity was detected in 2 of 11 thecomas, 1 of 11 SCTs, 4 of 10 SLCTs, 1 of 2 unclassified sex cord tumors, 1 of 10 FATPWOs, 4 of 12 SCCHCTs as well as in most germ cell tumors and epithelial-stromal tumors. 13 AGCTs, 11 JGCTs, 11 fibromas, 10 fibrosarcomas, 11 SSTs, 12 SCTATs, 1 gynandroblastoma, 9 steroid cell tumors, and 5 gonadoblastomas were HEA125 negative.

Conclusion

Our findings indicate that MIS is a marker of sex-cord differentiation and may be useful as a serum tumor marker for certain sex cord tumors, especially SCTAT. Although the detection of MIS and CD99 in some SCCHCTs and FATPWOs might argue in favor of a sex cord origin, the histogenesis of these tumors remains unclear. Although inhibin-α has previously been shown to be a more sensitive marker of sex-cord differentiation, a panel of immunohistochemical markers including MIS, CD99 and HEA125 may be helpful in the differential diagnosis of certain ovarian neoplasms.

Zusammenfassung

Zielsetzung

Die Expression von Müller-Gänge inhibierendem Hormon (MIS), CD99 und HEA125 ist von potenziellem Nutzen für die Differenzialdiagnostik der Ovarialtumoren.

Methodik

Ein Kollektiv von 179 Ovarialtumoren wurde mit monoklonalen oder polyklonalen Antikörpern und standardgemäßer immunhistochemischer Technik auf die Expression von MIS, CD99 und des epithelialen Markers HEA125 hin untersucht.

Ergebnisse

MIS war durchgehend in 9 primären und metastasierenden Sex cord Tumoren mit Ringtubuli (SCTAT) nachweisbar. 3 von 9 adulten Granulosazelltumoren (AGCT), 4 von 8 juvenilen Granulosazelltumoren (JGCT), 3 von 9 Sertolizelltumoren (SCT), 2 von 2 unklassifizierten Sex cord Tumoren, 2 von 7 Steroidzelltumoren, 1 Gonadoblastom, 3 von 8 Wolff'schen Tumoren (FATPWO) und 2 von 4 kleinzelligen hyperkalzämischen Ovarialkarzinomen (SCCHCT) waren ebenfalls MIS positiv. Demgegenüber waren 9 Thekome, 10 Fibrome, 10 Fibrosarkome, 8 sklerosierende Stromatumoren (SST) und 6 Sertoli-Leydigzelltumoren MIS negativ. Sämtliche 11 primären und metastasierenden JGCT waren CD99 positiv. Zusätzlich waren 4 von 13 AGCT, 3 von 11 Thekomen, 3 von 11 SST, 3 von 11 SCT, 2 von 10 SLCT, 2 von 12 SCTAT, 1 Gynandroblastom, 1 von 2 unklassifizierten Sex cord Tumoren und 4 von 12 SCCHCT CD99 positiv. Andererseits waren 11 Fibrome, 10 Fibrosarkome, 9 Steroidzelltumoren, 5 Gonadoblastome und 10 FATPWO CD99 negativ. Mit Ausnahme fokaler schwacher CD99 Immunreaktivität in 1 von 3 Dottersacktumoren (YST) waren alle 16 sonstigen Keimzelltumoren und sämtliche 18 epithelialen Borderline Tumoren und Karzinome CD99 negativ. HEA125 Expression wurde in 2 von 11 Thekomen, 1 von 11 SCT, 4 von 10 LCT, 1 von 2 unklassifizierten Sex cord Tumoren, 1 von 10 FATPWO, 4 von 12 SCCHCT sowie in den meisten Keimzelltumoren und epithelialen Tumoren nachgewiesen. 13 AGCT, 11 JGCT, 11 Fibrome, 10 Fibrosarkome, 11 SST, 12 SCTAT, 1 Gynandroblastom, 9 Steroidzelltumoren und 5 Gonadoblastome waren HEA125 negativ.

Schlussfolgerung

MIS ist ein Marker der Keimstrangdifferenzierung in Ovarialtumoren und kann potenziell als Tumormarker im Serum für Keimstrangtumoren (insbesondere SCTAT) eingesetzt werden. Wenngleich die Expression von MIS und CD99 in SCCHCT und FATPWO auf eine Herkunft dieser Tumoren von den Keimsträngen hindeuten könnte, bleibt deren Histogenese weiterhin ungeklärt. Obwohl Inhibin-α der im Vergleich zu MIS und CD99 sensiblere Marker für Keimstrangdifferenzierung ist, kann die Kombination der immunhistochemischen Marker MIS, CD99 und HEA125 in der Differenzialdiagnostik bestimmter Ovarialtumoren hilfreich sein.

Full Text

References

1 Aguirre P, Thor A D, Scully R E. Ovarian small cell carcinoma. Histogenetic considerations based on immunohistochemical and other findings. Am J Clin Pathol. 1989; 92 140-149
2 Bashir M S, Wells M. Müllerian inhibiting substance. J Pathol. 1995; 176 109-110
3 Chin T W, Parry R L, Donahoe P K. Human Müllerian inhibiting substance inhibits tumor growth in vitro and in vivo. Cancer Res. 1991; 51 2101-2106
4 Forest M G. Serum Müllerian inhibiting substance assay - a new diagnostic test for disorders of gonadal development. N Engl J Med. 1997; 336 1519-1521
5 Gordon M D, Corless C, Renshaw A A, Beckstead J. CD99, keratin, and vimentin staining of sex cord-stromal tumors, normal ovary, and testis. Mod Pathol. 1998; 11 769-773
6 Gustafson M L, Lee M M, Scully R E, Moncure A C, Hirakawa T, Goodman A. et al . Müllerian inhibiting substance as a marker for ovarian sex-cord tumor. N Engl J Med. 1992; 326 466-471
7 Hirobe S, He W W, Lee M M, Donahoe P K. Müllerian inhibiting substance messenger ribonucleic acid (mRNA) expression in granulosa and Sertoli cells coincides with their mitotic activity. Endocrinology. 1992; 131 854-862
8 Kommoss F, Oliva E, Bhan A K, Young R H, Scully R E. Inhibin expression in ovarian tumors and tumor-like lesions. An immunohistochemical study. Mod Pathol. 1998; 11 656-664
9 Kommoss F, Oliva E, Bittinger F, Kirkpatrick C J, Amin M B, Bhan A K. et al . Inhibin-α, CD99, HEA125, PLAP, and chromogranin immunoreactivity in testicular neoplasms and the androgen insensitivity syndrome. Hum Pathol. 2000; 31 1055-1061
10 Lane A H, Lee M M, Fuller A F, Kehas D J, Donahoe P K, MacLaughlin D T. Diagnostic utility of Müllerian inhibiting substance determination in patients with primary and recurrent granulosa cell tumors. Gynecol Oncol. 1999; 73 51-55
11 Lappöhn R E, Burger H G, Bouma J, Bangah M, Krans M, de Bruijn H W. Inhibin as a marker for granulosa-cell tumors. N Engl J Med. 1989; 321 790-793
12 Loo K T, Leung A K, Chan J K. Immunohistochemical staining of ovarian granulosa cell tumors with MIC2 antibody. Histopathology. 1995; 27 388-390
13 Matias-Guiu X, Pons C, Prat J. Müllerian inhibiting substance, alpha-inhibin, and CD99 expression in sex cord-stromal tumors and endometrioid carcinomas resembling sex cord-stromal tumors. Hum Pathol. 1998; 29 840-845
14 Moldenhauer G, Momburg F, Möller P, Schwartz R, Hammerling G J. Epithelium-specific surface glycoprotein of M_r 34, 000 is a widely distributed human carcinoma marker. Br J Cancer. 1987; 56 714-721
15 Momburg F, Moldenhauer G, Hämmerling G J, Möller P. Immunohistochemical study of the expression of a M_r 34, 000 human epithelium-specific surface glycoprotein in normal and malignant tissues. Cancer Res. 1987; 47 2883-2891
16 Puls L E, Hamous J H, Morrow M S, Schneyer A, MacLaughlin D T, Castracane V D. Recurrent ovarian sex cord tumor with annular tubules: Tumor marker and chemotherapy experience. Gynecol Oncol. 1994; 54 396-401
17 Riopel M A, Perlman E J, Seidman J D, Kurman R J, Sherman M E. Inhibin and epithelial membrane antigen immunohistochemistry assist in the diagnosis of sex cord-stromal tumors and provide clues to the histogenesis of hypercalcemic small cell carcinomas. Int J Gynecol Pathol. 1998; 17 46-53
18 Takahashi M, Koide S S, Donahoe P K. Müllerian inhibiting substance as an oocyte meiosis inhibitor. Mol Cell Endocrinol. 1986; 47 225-234
19 Ueno S, Takahashi M. Cellular localization of MIS in the developing rat ovary. Endocrinol. 1989; 124 1000-1006
20 Ulbright T M, Roth L M, Stehman F B, Talerman A, Senekjian E K. Poorly differentiated (small cell) carcinoma of the ovary in young women: Evidence supporting a germ cell origin. Hum Pathol. 1987; 18 175-184
21 Wallen J W, Cate R L, Kiefer D M, Riemen M W, Martinez D, Hoffman R M. et al . Minimal antiproliferative effect of recombinant Müllerian inhibiting substance on gynecological tumor cell lines and tumor explants. Cancer Res. 1989; 49 2005-2011
22 Weidner N, Tjoe J. Immunohistochemical profile of monoclonal antibody O13: Antibody that recognizes glycoprotein p30/30^MIC2 and is useful in diagnosing Ewing's sarcoma and peripheral neuroepithelioma. Am J Surg Pathol. 1994; 18 486-494
23 Whitman G F, Pantazis C G. Cellular localization of Müllerian inhibiting substance messenger ribonucleic acid during human ovarian follicular development. Am J Obstet Gynecol. 1991; 165 1881-1886
24 Yoon-La C, Hy-Sook K, Geunghwan A. Immunoexpression of inhibin α subunit, inhibin/activin βA subunit and CD99 in ovarian tumors. Arch Pathol Lab Med. 2000; 124 563-569
25 Young R H, Scully R E. Ovarian tumors of probable wolffian origin. Am J Surg Pathol. 1983; 7 125-135

Priv.-Doz. Dr. med. F. Kommoss

Institut für Pathologie
Referenzzentrum für Gynäkopathologie
A2,2

68159 Mannheim

Email: gyn-patho@t-online.de