癌症相关的可变剪接调控

Cancer-associated regulation of alternative splicing.

作者信息

Venables Julian P, Klinck Roscoe, Koh ChuShin, Gervais-Bird Julien, Bramard Anne, Inkel Lyna, Durand Mathieu, Couture Sonia, Froehlich Ulrike, Lapointe Elvy, Lucier Jean-François, Thibault Philippe, Rancourt Claudine, Tremblay Karine, Prinos Panagiotis, Chabot Benoit, Elela Sherif Abou

机构信息

Laboratoire de génomique fonctionnelle de l'Université de Sherbrooke, Sherbrooke, Québec, Canada.

出版信息

Nat Struct Mol Biol. 2009 Jun;16(6):670-6. doi: 10.1038/nsmb.1608. Epub 2009 May 17.

DOI:10.1038/nsmb.1608

PMID:19448617

Abstract

Alternative splicing of pre-mRNA increases the diversity of protein functions. Here we show that about half of all active alternative splicing events in ovarian and breast tissues are changed in tumors, and many seem to be regulated by a single factor; sequence analysis revealed binding sites for the RNA binding protein FOX2 downstream of one-third of the exons skipped in cancer. High-resolution analysis of FOX2 binding sites defined the precise positions relative to alternative exons at which the protein may function as either a silencer or an enhancer. Most of the identified targets were shifted in the same direction by FOX2 depletion in cell lines as they were in breast and ovarian cancer tissues. Notably, we found expression of FOX2 itself is downregulated in ovarian cancer and its splicing is altered in breast cancer samples. These results suggest that the decreased expression of FOX2 in cancer tissues modulates splicing and controls proliferation.

摘要

前体信使核糖核酸（pre-mRNA）的可变剪接增加了蛋白质功能的多样性。在此我们表明，卵巢组织和乳腺组织中约一半的活跃可变剪接事件在肿瘤中发生了改变，且许多似乎受单一因子调控；序列分析揭示，在癌症中跳过的三分之一外显子下游存在RNA结合蛋白FOX2的结合位点。对FOX2结合位点的高分辨率分析确定了其相对于可变外显子的精确位置，在这些位置该蛋白可能作为沉默子或增强子发挥作用。在细胞系中，大多数已鉴定的靶点因FOX2缺失而发生的变化方向与它们在乳腺癌和卵巢癌组织中的变化方向相同。值得注意的是，我们发现FOX2自身的表达在卵巢癌中下调，其剪接在乳腺癌样本中发生改变。这些结果表明，癌症组织中FOX2表达的降低会调节剪接并控制细胞增殖。

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癌症相关的可变剪接调控

Cancer-associated regulation of alternative splicing.

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