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癌症相关黏连蛋白变异对基因表达和细胞身份的功能影响。

Functional impact of cancer-associated cohesin variants on gene expression and cellular identity.

机构信息

Curriculum in Genetics and Molecular Biology, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599, USA.

Integrative Program for Biological and Genome Sciences, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599, USA.

出版信息

Genetics. 2021 Apr 15;217(4). doi: 10.1093/genetics/iyab025.

Abstract

Cohesin is a ring-shaped protein complex that controls dynamic chromosome structure. Cohesin activity is important for a variety of biological processes, including formation of DNA loops that regulate gene expression. The precise mechanisms by which cohesin shapes local chromosome structure and gene expression are not fully understood. Recurrent mutations in cohesin complex members have been reported in various cancers, though it is not clear whether many cohesin sequence variants have phenotypes and contribute to disease. Here, we utilized CRISPR/Cas9 genome editing to introduce a variety of cohesin sequence variants into murine embryonic stem cells and investigate their molecular and cellular consequences. Some of the cohesin variants tested caused changes to transcription, including altered expression of gene encoding lineage-specifying developmental regulators. Altered gene expression was also observed at insulated neighborhoods, where cohesin-mediated DNA loops constrain potential interactions between genes and enhancers. Furthermore, some cohesin variants altered the proliferation rate and differentiation potential of murine embryonic stem cells. This study provides a functional comparison of cohesin variants found in cancer within an isogenic system, revealing the relative roles of various cohesin perturbations on gene expression and maintenance of cellular identity.

摘要

黏连蛋白是一种环形蛋白复合物,可控制染色体的动态结构。黏连蛋白的活性对于多种生物学过程非常重要,包括形成调节基因表达的 DNA 环。黏连蛋白如何精确地塑造局部染色体结构和基因表达尚不完全清楚。黏连蛋白复合物成员的反复突变已在各种癌症中报道,但尚不清楚许多黏连蛋白序列变体是否具有表型并导致疾病。在这里,我们利用 CRISPR/Cas9 基因组编辑将各种黏连蛋白序列变体引入到鼠胚胎干细胞中,并研究它们的分子和细胞后果。测试的一些黏连蛋白变体导致转录发生变化,包括谱系特异性发育调节剂基因的表达改变。在隔离区也观察到了基因表达的改变,在那里,黏连蛋白介导的 DNA 环限制了基因和增强子之间潜在的相互作用。此外,一些黏连蛋白变体改变了鼠胚胎干细胞的增殖率和分化潜能。这项研究在同基因系统中对癌症中发现的黏连蛋白变体进行了功能比较,揭示了各种黏连蛋白扰动对基因表达和维持细胞特性的相对作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/20f2/8049558/b75919748995/iyab025f1.jpg

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