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Silencing by nuclear matrix attachment distinguishes cell-type specificity: association with increased proliferation capacity

机译:通过核基质附着沉默可区分细胞类型特异性:与增殖能力增强相关

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摘要

DNA loop organization by nuclear scaffold/matrix attachment is a key regulator of gene expression that may provide a means to modulate phenotype. We have previously shown that attachment of genes to the NaCl-isolated nuclear matrix correlates with their silencing in HeLa cells. In contrast, expressed genes were associated with the lithium 3,5-diiodosalicylate (LIS)-isolated nuclear scaffold. To define their role in determining phenotype matrix attached regions (MARs) on human chromosomes 14-18 were identified as a function of expression in a primary cell line. The locations of MARs in aortic adventitial fibroblast (AoAF) cells were very stable (r = 0.909) and 96% of genes attached at MARs are silent (P < 0.001). Approximately one-third of the genes uniquely expressed in AoAF cells were associated with the HeLa cell nuclear matrix and silenced. Comparatively, 81% were associated with the AoAF cell nuclear scaffold (P < 0.001) and expressed. This suggests that nuclear scaffold/matrix association mediates a portion of cell type-specific gene expression thereby modulating phenotype. Interestingly, nuclear matrix attachment and thus silencing of specific genes that regulate proliferation and maintain the integrity of the HeLa cell genome suggests that transformation may at least in part be achieved through aberrant nuclear matrix attachment.
机译:通过核支架/基质附着的DNA环组织是基因表达的关键调节因子,它可能提供调节表型的手段。先前我们已经表明,基因与NaCl分离的核基质的附着与其在HeLa细胞中的沉默相关。相反,表达的基因与3,5-二碘水杨酸锂(LIS)分离的核支架相关。为了确定它们在确定表型上的作用,确定了人类染色体14-18上的基质附着区(MARs)是原代细胞系中表达的函数。 MARs在主动脉外膜成纤维细胞(AoAF)细胞中的位置非常稳定(r = 0.909),并且在MARs附着的基因中有96%是沉默的(P <0.001)。在AoAF细胞中唯一表达的基因中大约有三分之一与HeLa细胞核基质相关并沉默了。比较而言,有81%与AoAF细胞核支架相关(P <0.001)并表达。这表明核支架/基质缔合介导了一部分细胞类型特异性基因表达,从而调节了表型。有趣的是,核基质附着以及因此调节增殖并维持HeLa细胞基因组完整性的特定基因的沉默表明,转化至少可以通过异常的核基质附着来实现。

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