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Deregulation of splicing factors and breast cancer development.

机译:放松剪接因子和乳腺癌发展的放松管制。

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It is well known that many genes implicated in the development and progression of breast cancer undergo aberrant alternative splicing events to produce proteins with pro-cancer properties. These changes in alternative splicing can arise from mutations or single-nucleotide polymorphisms (SNPs) within the DNA sequences of cancer-related genes, which can strongly affect the activity of splicing factors and influence the splice site choice. However, it is important to note that absence of mutations is not sufficient to prevent misleading choices in splice site selection. There is now increasing evidence to demonstrate that the expression profile of ten splicing factors (including SRs and hnRNPs) and eight RNA-binding proteins changes in breast cancer cells compared with normal cells. These modifications strongly influence the alternative splicing pattern of many cancer-related genes despite the absence of any detrimental mutations within their DNA sequences. Thus, a comprehensive assessment of the splicing factor status in breast cancer is important to provide insights into the mechanisms that lead to breast cancer development and metastasis. Whilst most studies focus on mutations that affect alternative splicing in cancer-related genes, this review focuses on splicing factors and RNA-binding proteins that are themselves deregulated in breast cancer and implicated in cancer-related alternative splicing events.
机译:众所周知,许多涉及乳腺癌发育和进展的许多基因经历了异常的替代剪接事件,以产生具有亲癌性质的蛋白质。替代剪接中的这些变化可能来自癌症相关基因的DNA序列内的突变或单核苷酸多态性(SNP),这可能强烈影响剪接因子的活性并影响剪接部位选择。然而,重要的是要注意,没有突变是不足以防止拼接位点选择中的误导性选择。现在存在越来越多的证据表明,与正常细胞相比,10个剪接因子(包括SRS和HNRNP)的表达谱和八个RNA结合蛋白在乳腺癌细胞中变化。这些修改强烈影响许多癌症相关基因的替代拼接模式,尽管在其DNA序列中没有任何有害突变。因此,对乳腺癌剪接因子状态的综合评估对于提供导致乳腺癌发育和转移的机制的见解是重要的。虽然大多数研究重点关注影响与癌症相关基因中的替代剪接的突变,但该综述侧重于剪接因子和RNA结合蛋白质,它们本身在乳腺癌中解除癌症,涉及与癌症相关的替代剪接事件。

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