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乳腺癌的基因进化:I. 细胞遗传学和DNA含量数据

Breast cancer genetic evolution: I. Data from cytogenetics and DNA content.

作者信息

Dutrillaux B, Gerbault-Seureau M, Remvikos Y, Zafrani B, Prieur M

机构信息

Institut Curie, Section de Biologie, URA 620 CNRS, Paris, France.

出版信息

Breast Cancer Res Treat. 1991 Nov;19(3):245-55. doi: 10.1007/BF01961161.

DOI:10.1007/BF01961161
PMID:1663804
Abstract

A general scheme of chromosome alterations occurring during tumor progression is proposed from the cytogenetic study of 113 breast carcinomas. For 76 of these tumors, chromosome numbers and rate of chromosome rearrangements were correlated with DNA content studied by flow cytometry. A series of 536 cases was used as control for flow cytometry. The following evolution can be proposed: 1. occurrence of unbalanced rearrangements decreasing chromosome number and DNA content; 2. correlatively to the rate of chromosome rearrangements, formation of endoreduplications leading to hyperploid sidelines; 3. persistence of the near diploid cells and decrease of chromosome number to about 35 and of DNA index to .85; 4. more frequently, elimination of the near diploid cells and complete passage to hyperploidy; 5. further losses of chromosomes in the hyperploid tumors, whose karyotypes can decrease to about 55 chromosomes and a DNA index of 1.35; 6. eventually, occurrence of a second endoreduplication, leading to an apparent near tetraploidy. The rate of rearranged chromosomes may reach 80% in both near diploid tumors with 35-40 and hyperploid tumors with 55-65 chromosomes which can be regarded as those with the highest degree of tumor progression. It is shown that the increase of chromosome number and DNA index above diploidy is very limited, and that all tumors with more than 50 chromosomes and 1.35 DNA content passed through endoreduplication. This results in many possible losses of heterozygosity in these cases.

摘要

通过对113例乳腺癌的细胞遗传学研究,提出了肿瘤进展过程中发生的染色体改变的一般模式。对于其中76例肿瘤,染色体数目和染色体重排率与通过流式细胞术研究的DNA含量相关。一系列536例病例用作流式细胞术的对照。可以提出以下演变过程:1. 发生不平衡重排,导致染色体数目和DNA含量减少;2. 与染色体重排率相关,形成核内复制,导致超二倍体旁系细胞形成;3. 近二倍体细胞持续存在,染色体数目减少至约35条,DNA指数降至0.85;4. 更常见的是,近二倍体细胞被消除并完全转变为超二倍体;5. 超二倍体肿瘤中进一步的染色体丢失,其核型可减少至约55条染色体,DNA指数为1.35;6. 最终,发生第二次核内复制,导致明显的近四倍体。在染色体数目为35 - 40条的近二倍体肿瘤和染色体数目为55 - 65条的超二倍体肿瘤中,重排染色体的比例可能达到80%,这些肿瘤可被视为肿瘤进展程度最高的肿瘤。结果表明,染色体数目和DNA指数高于二倍体的增加非常有限,并且所有染色体数目超过50条且DNA含量大于1.35的肿瘤都经历了核内复制。这导致在这些情况下许多可能的杂合性丢失。

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