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使用iCLIP以核苷酸分辨率分析RNA结合蛋白的结合位点

Profiling the Binding Sites of RNA-Binding Proteins with Nucleotide Resolution Using iCLIP.

作者信息

Sutandy F X Reymond, Hildebrandt Andrea, König Julian

机构信息

Institute of Molecular Biology gGmbH, Ackermannweg 4, 55128, Mainz, Germany.

出版信息

Methods Mol Biol. 2016;1358:175-95. doi: 10.1007/978-1-4939-3067-8_11.

Abstract

The importance of posttranscriptional regulation in cellular metabolism has recently gone beyond what was previously appreciated. The regulatory mechanisms are controlled by RNA-binding proteins (RBPs), which form complexes with RNA and regulate RNA processing, stability, and localization, among others. Consistently, mutations in RBPs result in defects in developmental processes, diseases, and cancer. Gaining deeper insights into the biology of RNA-RBP interactions will lead to a better understanding of regulatory processes and disease development. Several techniques have been developed to capture the properties of RNA-RBP interactions. Furthermore, the development of high-throughput sequencing has broadened the capability of these methods. Here, we summarize individual-nucleotide resolution UV cross-linking and immunoprecipitation (iCLIP), a powerful technique that provides genome-wide information on RNA-RBP interactions at nucleotide resolution. In this chapter, we outline the iCLIP protocol and list possible controls that allow a targeted and cost-minimizing optimization of the protocol for an RBP-of-interest. Moreover, we provide notes on experimental design and a troubleshooting guideline for common problems that can occur during iCLIP library preparation.

摘要

转录后调控在细胞代谢中的重要性近来已超出了以往的认知。调控机制由RNA结合蛋白(RBPs)控制,这些蛋白与RNA形成复合物,并调节RNA加工、稳定性和定位等。一致地,RBPs中的突变会导致发育过程、疾病和癌症中的缺陷。更深入地了解RNA-RBP相互作用的生物学特性将有助于更好地理解调控过程和疾病发展。已经开发了几种技术来捕捉RNA-RBP相互作用的特性。此外,高通量测序的发展拓宽了这些方法的能力。在这里,我们总结了单核苷酸分辨率紫外线交联免疫沉淀(iCLIP),这是一种强大的技术,可在核苷酸分辨率上提供全基因组范围内关于RNA-RBP相互作用的信息。在本章中,我们概述了iCLIP方案,并列出了可能的对照,这些对照允许针对感兴趣的RBP对方案进行有针对性且成本最小化的优化。此外,我们提供了关于实验设计的说明以及iCLIP文库制备过程中可能出现的常见问题的故障排除指南。

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