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卵巢腺癌细胞系中9号染色体短臂的纯合缺失以及散发性肿瘤中的杂合性缺失。

Homozygous deletions on the short arm of chromosome 9 in ovarian adenocarcinoma cell lines and loss of heterozygosity in sporadic tumors.

作者信息

Chenevix-Trench G, Kerr J, Friedlander M, Hurst T, Sanderson B, Coglan M, Ward B, Leary J, Khoo S K

机构信息

Queensland Cancer Fund Research Unit, Queensland Institute of Medical Research, Brisbane, Australia.

出版信息

Am J Hum Genet. 1994 Jul;55(1):143-9.

Abstract

Rat ovarian surface epithelial cells transformed spontaneously in vitro have been found to have homozygous deletions of the interferon alpha (IFNA) gene. This suggests that inactivation of a tumor-suppressor gene in this region may be crucial for the development of ovarian cancer. We therefore used microsatellite markers and Southern analysis to examine the homologous region in humans--the short arm of chromosome 9--for deletions in sporadic ovarian adenocarcinomas and ovarian tumor cell lines. Loss of heterozygosity occurred in 34 (37%) of 91 informative sporadic tumors, including some benign, low-malignant-potential and early-stage tumors, suggesting that it is an early event in the development of ovarian adenocarcinoma. Furthermore, homozygous deletions on 9p were found in 2 of 10 independent cell lines. Deletion mapping of the tumors and lines indicates that the candidate suppressor gene inactivated as a consequence lies between D9S171 and the IFNA locus, a region that is also deleted in several other tumors and that contains the melanoma predisposition gene, MLM.

摘要

已发现体外自发转化的大鼠卵巢表面上皮细胞存在干扰素α(IFNA)基因的纯合缺失。这表明该区域肿瘤抑制基因的失活可能对卵巢癌的发生发展至关重要。因此,我们使用微卫星标记和Southern分析来检测人类的同源区域——9号染色体短臂——在散发性卵巢腺癌和卵巢肿瘤细胞系中是否存在缺失。在91例信息充分的散发性肿瘤中有34例(37%)发生杂合性缺失,包括一些良性、低恶性潜能和早期肿瘤,这表明杂合性缺失是卵巢腺癌发生发展过程中的早期事件。此外,在10个独立细胞系中有2个发现9p上存在纯合缺失。对肿瘤和细胞系的缺失定位表明,由此失活的候选抑癌基因位于D9S171和IFNA基因座之间,该区域在其他几种肿瘤中也有缺失,并且包含黑色素瘤易感基因MLM。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/35e7/1918224/62a408c793d3/ajhg00040-0150-a.jpg

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