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无论TP53突变状态如何,MDM2过表达在卵巢癌中都很罕见。

MDM2 overexpression is rare in ovarian carcinoma irrespective of TP53 mutation status.

作者信息

Foulkes W D, Stamp G W, Afzal S, Lalani N, McFarlane C P, Trowsdale J, Campbell I G

机构信息

Department of Medicine, Montreal General Hospital, QC, Canada.

出版信息

Br J Cancer. 1995 Oct;72(4):883-8. doi: 10.1038/bjc.1995.428.

Abstract

Somatic mutations in TP53 are seen in many human cancers. In addition, the protein product of the wild-type TP53 can be sequestered by the protein MDM2 (murine double minute 2). This protein is commonly overexpressed in human sarcomas and gliomas, usually as a result of gene amplification. In this study, 43 ovarian carcinomas (OCs) were analysed for aberrations in the TP53 gene by immunohistochemistry (IHC), loss of heterozygosity (LOH) or mutation analysis. The MDM2 gene and its product was studied by Southern blotting and IHC. Over 50% of the OCs studied showed mutations in TP53 by either direct sequencing (19/36, 53%), positive IHC (23,43, 53%) or both, whereas 0/32 had amplification of MDM2 and only 1/37 tumours had positive IHC using the anti-MDM2 antibody IF-2. The solitary example of positive IHC in this series was seen in a mixed müllerian tumour with sarcomatous differentiation and was not accompanied by MDM2 DNA amplification. These results support previous data showing that around 50% of OCs have mutations in TP53 and in addition, suggest that MDM2 is not amplified in OC, but the presence of sarcomatous features in mixed müllerian tumours may result in positive immunohistochemistry with IF-2.

摘要

TP53基因的体细胞突变在许多人类癌症中都有发现。此外,野生型TP53的蛋白质产物可被MDM2(小鼠双微体2)蛋白所隔离。这种蛋白质在人类肉瘤和神经胶质瘤中通常过度表达,通常是基因扩增的结果。在本研究中,通过免疫组织化学(IHC)、杂合性缺失(LOH)或突变分析,对43例卵巢癌(OC)的TP53基因畸变进行了分析。通过Southern印迹法和免疫组织化学对MDM2基因及其产物进行了研究。超过50%的研究卵巢癌通过直接测序(19/36,53%)、免疫组织化学阳性(23/43,53%)或两者兼而有之显示TP53突变,而32例中0例有MDM2扩增,使用抗MDM2抗体IF-2时只有1/37的肿瘤免疫组织化学呈阳性。该系列中免疫组织化学阳性的唯一例子见于一例伴有肉瘤样分化的混合性苗勒管肿瘤,且未伴有MDM2 DNA扩增。这些结果支持了先前的数据,即约50%的卵巢癌有TP53突变,此外,提示MDM2在卵巢癌中未扩增,但混合性苗勒管肿瘤中肉瘤样特征的存在可能导致IF-2免疫组织化学呈阳性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f36/2034047/97c61e69e09d/brjcancer00044-0085-a.jpg

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