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Gene regulation by SMAR1: Role in cellular homeostasis and cancer.

机译:SMAR1的基因调控:在细胞稳态和癌症中的作用。

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Changes in the composition of nuclear matrix associated proteins contribute to alterations in nuclear structure, one of the major phenotypes of malignant cancer cells. The malignancy-induced changes in this structure lead to alterations in chromatin folding, the fidelity of genome replication and gene expression programs. The nuclear matrix forms a scaffold upon which the chromatin is organized into periodic loop domains called matrix attachment regions (MAR) by binding to various MAR binding proteins (MARBPs). Aberrant expression of MARBPs modulates the chromatin organization and disrupt transcriptional network that leads to oncogenesis. Dysregulation of nuclear matrix associated MARBPs has been reported in different types of cancers. Some of these proteins have tumor specific expression and are therefore considered as promising diagnostic or prognostic markers in few cancers. SMAR1 (scaffold/matrix attachment region binding protein 1), is one such nuclear matrix associated protein whose expression is drastically reduced in higher grades of breast cancer. SMAR1 gene is located on human chromosome 16q24.3 locus, the loss of heterozygosity (LOH) of which has been reported in several types of cancers. This review elaborates on the multiple roles of nuclear matrix associated protein SMAR1 in regulating various cellular target genes involved in cell growth, apoptosis and tumorigenesis.
机译:核基质相关蛋白组成的变化有助于改变核结构,这是恶性癌细胞的主要表型之一。恶性肿瘤引起的这种结构改变导致染色质折叠,基因组复制和基因表达程序的保真度发生变化。核基质形成一个支架,在该支架上,染色质通过与各种MAR结合蛋白(MARBP)结合而被组织成称为基质附着区(MAR)的周期性环结构域。 MARBPs的异常表达调节染色质组织并破坏导致肿瘤发生的转录网络。已经报道了在不同类型的癌症中与核基质相关的MARBP的失调。这些蛋白质中的一些具有肿瘤特异性表达,因此被认为是极少数癌症中有希望的诊断或预后标志物。 SMAR1(支架/基质附着区结合蛋白1)是一种这样的核基质相关蛋白,在较高等级的乳腺癌中其表达急剧降低。 SMAR1基因位于人类染色体16q24.3位点,其杂合性缺失(LOH)已在几种类型的癌症中报告。这篇综述详细阐述了核基质相关蛋白SMAR1在调节参与细胞生长,凋亡和肿瘤发生的各种细胞靶基因中的多种作用。

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