Loss of ARID1B and SMARCB1 expression are specific for the diagnosis of dedifferentiated/undifferentiated carcinoma in tumours of the upper gynaecological tract and cervix
Aims Genomic inactivation of ARID1B in ARID1A-inactivated tumour and genomic inactivation of SMARCB1 represent two recurrent mechanisms, core SWItch/sucrose non-fermentable (SWI/SNF) complex inactivation, that are associated with de-differentiation in endometrial carcinoma. Approximately one-third of dedifferentiated/undifferentiated endometrial carcinomas (DDEC/UEC) show loss of ARID1B expression with a minor subset showing loss of SMARCB1 expression, but little is known regarding the specificity of ARID1B or SMARCB1 loss in gynaecological tract tumours in general. The aim of this study was to examine the frequency of ARID1B and SMARCB1 loss by immunohistochemistry in a series of gynaecological tract epithelial/mesenchymal neoplasms. Methods and results We evaluated 1849 tumours that included 748 endometrial carcinomas, 101 uterine carcinosarcomas/adenosarcomas, 64 uterine sarcomas, 221 cervical carcinomas and 715 ovarian carcinomas/borderline tumours by tissue microarrays (TMA). We observed ARID1B loss in 35 of 86 (41%) and SMARCB1 loss in three of 86 (3%) DDEC/UEC, but not in any other uterine tumour types examined. ARID1B-deficient DDEC/UEC also showed concurrent loss of ARID1A expression. All SMARCB1-deficient tumours showed loss of MLH1 and PMS2, while 29 of 35 ARID1B-deficient tumours showed loss of MLH1 and PMS2 or loss of MSH6. All ovarian carcinomas/borderline tumours and cervical carcinomas showed intact expression of ARID1B and SMARCB1. Conclusion Our findings indicate that the loss of expression of ARID1B or SMARCB1 by immunohistochemistry is highly specific for undifferentiated carcinoma among tumours of the upper gynaecological tract and cervix, and therefore can be used to identify these highly aggressive malignant tumours.
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Ambroise Pare Hosp, AP HP, Dept Pathol, Boulogne, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Melloul, S.
Mosnier, J-F
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Hop Hotel Dieu, Dept Pathol, Nantes, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Mosnier, J-F
Masliah-Planchon, J.
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Inst Curie, Somat Genet Unit, Paris, France
INSERMU830, Inst Curie, Paris Sci Lettres, Res Ctr, Paris, France
Inst Curie, SIREDO, Paris, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Masliah-Planchon, J.
Lepage, C.
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Francois Mitterrand Univ Hosp, Dijon, France
Univ Burgundy & Franche Comte, EPICAD INSERM LNC UMR 1231, Besancon, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Lepage, C.
Le Malicot, K.
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Univ Burgundy & Franche Comte, EPICAD INSERM LNC UMR 1231, Besancon, France
Francophone Soc Digest Canc, Dijon, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Le Malicot, K.
Gornet, J-M
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St Louis Hosp, AP HP, Paris, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Gornet, J-M
Edeline, J.
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Eugene Marquis Ctr, Rennes, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Edeline, J.
Dansette, D.
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Hop Hotel Dieu, Dept Pathol, Nantes, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Dansette, D.
Texereau, P.
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Layne Hosp Ctr, Mt De Marsan, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Texereau, P.
Delattre, O.
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Inst Curie, Somat Genet Unit, Paris, France
INSERMU830, Inst Curie, Paris Sci Lettres, Res Ctr, Paris, France
Inst Curie, SIREDO, Paris, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Delattre, O.
Puig, P. Laurent
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G Pompidou European Hosp, AP HP, Paris, France
INSERM UMR S1147, Paris, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Puig, P. Laurent
Taieb, J.
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G Pompidou European Hosp, AP HP, Paris, France
INSERM UMR S1147, Paris, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Taieb, J.
Emile, J-F
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Ambroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France
Paris Saclay Univ, Versailles SQY Univ, EA4340 BCOH, Boulogne, FranceAmbroise Pare Hosp, AP HP, Dept Pathol, Boulogne, France