Chromosome abnormalities in human leukemia as indicators of mutagenic exposure.

J D Rowley
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Abstract

It is from an analysis of these data that I proposed that losses of all or part of the long arm of chromosomes 5 and/or 7 may be indicators of exposure to mutagenic agents (8). Moreover, our analysis of the regions of chromosomes 5 and 7 that are consistently missing can define the critical region of each chromosome with some precision. Looked at from another perspective, the frequency of losses of chromosomes 5 and/or 7 may be an indicator of the proportion of ANLL in each particular population that is related to some mutagenic exposure. These aberrations are most frequent in cells of patients who were previously exposed to various cytotoxic regimens for treatment of a primary (usually malignant) disease; these patients are considered to have 2 degrees ANLL. Among patients with ANLL de novo, abnormalities of chromosomes 5 and 7 are much more frequent in older than younger patients. Finally, among adult patients with ANLL de novo, -5 and -7 are more common in those whose occupations could potentially expose them to mutagenic agents such as chemicals, pesticides, or petroleum products. With regard to chromosome 5, most of these deletions are interstitial and always include 5q23 through q31, which I have called the critical region. Although I am less certain with regard to chromosome 7, it appears that the critical region that is consistently deleted may be 7q32 or 7q34-35.

人类白血病染色体异常作为诱变暴露的指标。
正是通过对这些数据的分析,我提出,5号染色体和/或7号染色体长臂的全部或部分缺失可能是暴露于诱变剂的指标(8)。此外,我们对5号染色体和7号染色体持续缺失区域的分析可以一定程度上精确地定义每条染色体的关键区域。从另一个角度来看,5号和/或7号染色体丢失的频率可能是每个特定人群中与某些诱变暴露有关的ANLL比例的一个指标。这些畸变最常见于以前为治疗原发性(通常是恶性)疾病而暴露于各种细胞毒性方案的患者的细胞中;这些患者被认为是2度ANLL。在新生ANLL患者中,5号和7号染色体的异常在老年患者中比年轻患者更常见。最后,在新生ANLL的成年患者中,-5和-7在那些职业可能暴露于致突变剂(如化学品、杀虫剂或石油产品)的人群中更为常见。关于5号染色体,大多数这些缺失是间隙性的,并且总是包括5q23到q31,我称之为关键区域。虽然我对7号染色体不太确定,但似乎一直被删除的关键区域可能是7q32或7q34-35。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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