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多灶性和双侧乳腺肿瘤克隆性的分子研究。

Molecular study of clonality in multifocal and bilateral breast tumors.

作者信息

Chunder Neelanjana, Roy Anup, Roychoudhury Susanta, Panda Chinmay Kumar

机构信息

Department of Oncogene Regulation, Chittaranjan National Cancer Institute, 37, S.P. Mukherjee Road, Kolkata-700026, India.

出版信息

Pathol Res Pract. 2004;200(10):735-41. doi: 10.1016/j.prp.2004.09.001.

Abstract

The clonal origin of multiple tumors in the same individual has long been debated. The main aim of this study is to find out whether multiple tumors in same individuals originated from a single clone. In our previous work (Pathol. Res. Pract. 199 (2003) 313-321), the deletion at chromosome1p36 was found to occur early because of common allelic loss in the bilateral tumors. In order to further investigate the findings about the clonality of tumors, eight tumors from four patients (two synchronous bilateral breast carcinoma [biBC], one case with breast carcinoma in one breast and multiple calcified fibroadenoma nodules in another breast, and one case with multifocal fibroadenosis in one breast) were subjected to polymerase chain reaction (PCR) to detect (a) loss of heterozygosity (LOH) and microsatellite size alterations (MA) using microsatellite markers distributed over five chromosomal arms 11p/q, 13q and 17p/q, and (b) Cyclin D1 amplification. Some markers were intragenic for BRCA1, BRCA2, BRCAX, ATM, TP53, and RB1. Although a few cases were studied, our findings suggest that in at least a proportion of patients multiple tumors may arise from a single clone.

摘要

同一患者体内多个肿瘤的克隆起源长期以来一直存在争议。本研究的主要目的是查明同一患者体内的多个肿瘤是否起源于单个克隆。在我们之前的研究(《病理学研究与实践》199卷,2003年,第313 - 321页)中,发现1号染色体p36区域的缺失发生较早,原因是双侧肿瘤存在共同的等位基因缺失。为了进一步研究肿瘤克隆性的相关发现,对4例患者的8个肿瘤(2例同步双侧乳腺癌[biBC],1例一侧乳腺为乳腺癌,另一侧乳腺有多个钙化纤维腺瘤结节,1例一侧乳腺有多灶性纤维腺病)进行聚合酶链反应(PCR),以检测:(a)使用分布在11p/q、13q和17p/q五条染色体臂上的微卫星标记检测杂合性缺失(LOH)和微卫星大小改变(MA);(b)细胞周期蛋白D1扩增。一些标记位于BRCA1、BRCA2、BRCAX、ATM、TP53和RB1基因内部。尽管仅研究了少数病例,但我们的研究结果表明,至少在一部分患者中,多个肿瘤可能起源于单个克隆。

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