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快速反应剪接报告基因筛选鉴定组成性剪接和选择性剪接的差异调控因子。

Rapid-response splicing reporter screens identify differential regulators of constitutive and alternative splicing.

机构信息

Howard Hughes Medical Institute, Department of Biochemistry and Biophysics, University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania 19104-6148, USA.

出版信息

Mol Cell Biol. 2010 Apr;30(7):1718-28. doi: 10.1128/MCB.01301-09. Epub 2010 Feb 1.

Abstract

Bioactive compounds have been invaluable for dissecting the mechanisms, regulation, and functions of cellular processes. However, very few such reagents have been described for pre-mRNA splicing. To facilitate their systematic discovery, we developed a high-throughput cell-based assay that measures pre-mRNA splicing by utilizing a quantitative reporter system with advantageous features. The reporter, consisting of a destabilized, intron-containing luciferase expressed from a short-lived mRNA, allows rapid screens (<4 h), thereby obviating the potential toxicity of splicing inhibitors. We describe three inhibitors (out of >23,000 screened), all pharmacologically active: clotrimazole, flunarizine, and chlorhexidine. Interestingly, none was a general splicing inhibitor. Rather, each caused distinct splicing changes of numerous genes. We further discovered the target of action of chlorhexidine and show that it is a selective inhibitor of specific Cdc2-like kinases (Clks) that phosphorylate serine-arginine-rich (SR) protein splicing factors. Our findings reveal unexpected activities of clinically used drugs in splicing and uncover differential regulation of constitutively spliced introns.

摘要

生物活性化合物在剖析细胞过程的机制、调控和功能方面具有不可估量的价值。然而,用于前体 mRNA 剪接的此类试剂却非常少。为了促进它们的系统发现,我们开发了一种高通量基于细胞的测定法,该方法利用具有优势特征的定量报告基因系统来测量前体 mRNA 剪接。该报告基因由一个不稳定的、包含内含子的 luciferase 组成,由半衰期短的 mRNA 表达,允许快速筛选(<4 小时),从而避免了剪接抑制剂的潜在毒性。我们描述了三种抑制剂(在>23,000 种筛选的化合物中),全部具有药理活性:克霉唑、氟桂利嗪和氯己定。有趣的是,没有一种是通用的剪接抑制剂。相反,每种抑制剂都会导致许多基因的剪接发生明显变化。我们进一步发现了氯己定的作用靶点,并表明它是一种选择性的 Cdc2 样激酶(Clks)抑制剂,Clks 会磷酸化丝氨酸-精氨酸丰富(SR)蛋白剪接因子。我们的发现揭示了临床使用药物在剪接中的意外活性,并揭示了组成性剪接内含子的差异调控。

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