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原发性膀胱癌中14号染色体长臂上的新型抑制基因座。

Novel suppressor loci on chromosome 14q in primary bladder cancer.

作者信息

Chang W Y, Cairns P, Schoenberg M P, Polascik T J, Sidransky D

机构信息

Department of Otolaryngology-Head and Neck Surgery, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205, USA.

出版信息

Cancer Res. 1995 Aug 1;55(15):3246-9.

PMID:7614456
Abstract

Two hundred eighty-five primary human carcinomas of the urinary bladder were examined for allelic loss on chromosome 14q. Seventeen highly polymorphic dinucleotide markers spanning the long arm of this acrocentric chromosome were selected for fine PCR-based mapping. Loss of heterozygosity for at least one marker was observed in 72 (25.3%) tumors. Thirty-four of these 72 tumors (47.2%) lost the entire long arm (monosomy), as suggested by loss of heterozygosity at all informative sites. Allelic loss on 14q occurred in all grades and stages of bladder cancer but was more commonly associated with muscle-invasive tumors (Ta, 9.4%; T1, 24.1%; and > or = T2, 41%). A deletion map of 16 primary tumors with partial losses delineated two minimal regions of loss. One region (approximately 2 cM) was bounded by markers D14S75 and D14S288 and the other (approximately 3 cM) by D14S51 and D14S267. Our results demonstrate that 14q loss is common in invasive bladder cancer and suggest that two potential suppressor loci at 14q12 and 14q32.1-32.2 may contribute to the genetic progression of this common cancer.

摘要

对285例原发性人类膀胱癌进行了14号染色体长臂上等位基因缺失检测。选择了17个高度多态性的二核苷酸标记,用于对这条近端着丝粒染色体长臂进行精细的基于PCR的定位。在72例(25.3%)肿瘤中观察到至少一个标记的杂合性缺失。这72例肿瘤中有34例(47.2%)丢失了整个长臂(单体型),所有信息位点的杂合性缺失提示了这一点。14号染色体长臂上的等位基因缺失在膀胱癌的所有分级和分期中均有发生,但更常见于肌层浸润性肿瘤(Ta期,9.4%;T1期,24.1%;T2期及以上,41%)。对16例有部分缺失的原发性肿瘤进行的缺失图谱分析确定了两个最小缺失区域。一个区域(约2 cM)由标记D14S75和D14S288界定,另一个区域(约3 cM)由D14S51和D14S267界定。我们的结果表明,14号染色体长臂缺失在浸润性膀胱癌中很常见,并提示14q12和14q32.1 - 32.2处的两个潜在抑癌基因座可能参与了这种常见癌症的遗传进展。

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