Chromosome breakage syndromes and cancer.

Nahum J Duker
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引用次数: 67

Abstract

There exist numerous genetic disorders, marked by chromosome instability, that are strikingly associated with various cancers. Both the chromosomal instabilities and neoplastic outcomes are related to abnormalities of DNA metabolism, DNA repair, cell-cycle governance, or control of apoptosis. Among these diseases are ataxia telangectasia and Nijmegen breakage syndrome, with increased incidences of lymphomas. Bloom syndrome, Werner syndrome, and Rothmund-Thompson syndrome, each characterized by a DNA helicase defect, are associated with early incidences of different cancers. Other diseases combining the phenotype of chromosomal instabilities and neoplastic development are Fanconi anemia and breast cancers associated with mutant BRCA1 and BRCA2 genes. The cloning of the encoding genes and the characterization of their products have resulted in partial understanding of the pathways of cellular DNA surveillance and maintenance of genomic rectitude. The exact pathways fully linking the genetic defect mechanisms to the eventual development of various neoplasias remain to be elucidated, but progress in defining the molecular genetics of these entities suggests that many of them are disorders of DNA recombination. Each defect involves a separate protein in these complex pathways.

染色体断裂综合征和癌症。
存在着许多以染色体不稳定为特征的遗传疾病,它们与各种癌症有着惊人的联系。染色体不稳定性和肿瘤结果都与DNA代谢、DNA修复、细胞周期治理或细胞凋亡控制的异常有关。这些疾病包括共济失调性毛细血管扩张症和奈梅亨断裂综合征,淋巴瘤的发病率增加。Bloom综合征、Werner综合征和rothmond - thompson综合征都以DNA解旋酶缺陷为特征,它们与不同癌症的早期发病率有关。其他结合染色体不稳定表型和肿瘤发展的疾病有范可尼贫血和与BRCA1和BRCA2基因突变相关的乳腺癌。编码基因的克隆及其产物的表征使我们对细胞DNA监视和基因组完整性维持的途径有了部分的了解。遗传缺陷机制与各种肿瘤最终发展的确切途径仍有待阐明,但在定义这些实体的分子遗传学方面的进展表明,其中许多是DNA重组障碍。在这些复杂的途径中,每个缺陷都涉及一个单独的蛋白质。
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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