首页> 美国卫生研究院文献>Oncotarget >Chromosome nondisjunction during bipolar mitoses of binucleated intermediates promote aneuploidy formation along with multipolar mitoses rather than chromosome loss in micronuclei induced by asbestos
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Chromosome nondisjunction during bipolar mitoses of binucleated intermediates promote aneuploidy formation along with multipolar mitoses rather than chromosome loss in micronuclei induced by asbestos

机译:双核中间体双极性有丝分裂期间的染色体非分离促进了多极性有丝分裂的非整倍体形成而不是石棉引起的微核中的染色体丢失

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摘要

Asbestos is a well-known occupational carcinogen that can cause aneuploidy during the early stages of neoplastic development. To explore the origins of asbestos-induced aneuploidy, we performed long-term live-cell imaging followed by fluorescence in situ hybridization of chromosomes 8 and 12 in human bronchial epithelial (HBEC) and mesothelial (MeT5A) cells. We demonstrate that asbestos induces aneuploidy via binucleated intermediates resulting from cytokinesis failure. On the one hand, asbestos increases chromosome nondisjunction during bipolar divisions of binucleated intermediates and produces near-tetraploidy. On the other hand, asbestos increases multipolar divisions of binucleated intermediates to produce aneuploidy. Surprisingly, chromosomes in asbestos-induced micronucleated cells are not truly lost by the cells, and do not contribute to aneuploid cell formation in either cell type. These results clarify the cellular source of asbestos-induced aneuploidy. In particular, they show the asbestos-induced disruption of bipolar chromosomal segregation in tetraploid cells, thereby demonstrating the causality between binucleated intermediates and aneuploidy evolution, rather than chromosome loss in micronuclei.
机译:石棉是一种众所周知的职业致癌物,可在肿瘤发展的早期阶段引起非整倍性。为了探索石棉诱导的非整倍性的起源,我们进行了长期的活细胞成像,然后在人支气管上皮细胞(HBEC)和间皮细胞(MeT5A)中进行了染色体8和12的荧光原位杂交。我们证明石棉通过胞质分裂失败所致的双核中间体诱导非整倍体。一方面,石棉会在双核中间体的双极分裂过程中增加染色体不分离,并产生近四倍体。另一方面,石棉增加了双核中间体的多极分裂,从而产生非整倍性。令人惊讶的是,石棉诱导的微核细胞中的染色体并没有真正被细胞丢失,并且在两种细胞类型中都不有助于非整倍体细胞的形成。这些结果阐明了石棉诱导的非整倍性的细胞来源。特别是,它们显示了石棉诱导的四倍体细胞中双极染色体分离的破坏,从而证明了双核中间体与非整倍性进化之间的因果关系,而不是微核中的染色体损失。

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