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染色体错误分离对基因组稳定性的短期分子后果。

Short-term molecular consequences of chromosome mis-segregation for genome stability.

机构信息

Department of Experimental Oncology at IEO, European Institute of Oncology IRCCS, Via Adamello 16, 20139, Milan, Italy.

IFOM ETS - The AIRC Institute of Molecular Oncology, via Adamello 16, 20139, Milan, Italy.

出版信息

Nat Commun. 2023 Mar 11;14(1):1353. doi: 10.1038/s41467-023-37095-7.

Abstract

Chromosome instability (CIN) is the most common form of genome instability and is a hallmark of cancer. CIN invariably leads to aneuploidy, a state of karyotype imbalance. Here, we show that aneuploidy can also trigger CIN. We found that aneuploid cells experience DNA replication stress in their first S-phase and precipitate in a state of continuous CIN. This generates a repertoire of genetically diverse cells with structural chromosomal abnormalities that can either continue proliferating or stop dividing. Cycling aneuploid cells display lower karyotype complexity compared to the arrested ones and increased expression of DNA repair signatures. Interestingly, the same signatures are upregulated in highly-proliferative cancer cells, which might enable them to proliferate despite the disadvantage conferred by aneuploidy-induced CIN. Altogether, our study reveals the short-term origins of CIN following aneuploidy and indicates the aneuploid state of cancer cells as a point mutation-independent source of genome instability, providing an explanation for aneuploidy occurrence in tumors.

摘要

染色体不稳定(CIN)是最常见的基因组不稳定形式,是癌症的标志。CIN 总是导致非整倍体,即核型失衡的状态。在这里,我们表明非整倍体也可以引发 CIN。我们发现,非整倍体细胞在其第一个 S 期经历 DNA 复制应激,并沉淀在持续 CIN 的状态中。这产生了一系列具有结构染色体异常的遗传多样性细胞,这些细胞可以继续增殖或停止分裂。与停滞的细胞相比,有丝分裂非整倍体细胞的核型复杂性降低,并且 DNA 修复特征的表达增加。有趣的是,在高度增殖的癌细胞中同样的特征上调,这可能使它们能够增殖,尽管非整倍体诱导的 CIN 带来了不利影响。总的来说,我们的研究揭示了非整倍体后 CIN 的短期起源,并表明癌细胞的非整倍体状态是基因突变独立的基因组不稳定的来源,为肿瘤中非整倍体的发生提供了一种解释。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/85c9/10008630/e04c8f666ec0/41467_2023_37095_Fig1_HTML.jpg

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