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HI-C 2.0: AN OPTIMIZED HI-C PROCEDURE FOR HIGH-RESOLUTION GENOME-WIDE MAPPING OF CHROMOSOME CONFORMATION

机译:HI-C 2.0:高分辨率的染色体组构图的全基因组映射的优化HI-C程序

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摘要

Chromosome conformation capture-based methods such as Hi-C have become mainstream techniques for the study of the 3D organization of genomes. These methods convert chromatin interactions reflecting topological chromatin structures into digital information (counts of pair-wise interactions). Here, we describe an updated protocol for Hi-C (Hi-C 2.0) that integrates recent improvements into a single protocol for efficient and high-resolution capture of chromatin interactions. This protocol combines chromatin digestion and frequently cutting enzymes to obtain kilobase (Kb) resolution. It also includes steps to reduce random ligation and the generation of uninformative molecules, such as unligated ends, to improve the amount of valid intra-chromosomal read pairs. This protocol allows for obtaining information on conformational structures such as compartment and topologically associating domains, as well as high-resolution conformational features such as DNA loops.
机译:基于染色体构象捕获的方法(例如Hi-C)已成为研究基因组3D组织的主流技术。这些方法将反映拓扑染色质结构的染色质相互作用转换为数字信息(成对相互作用的计数)。在这里,我们描述了Hi-C(Hi-C 2.0)的更新协议,该协议将最新的改进集成到单个协议中,以高效,高分辨率地捕获染色质相互作用。该协议结合了染色质消化和经常切割酶以获得千碱基(Kb)分辨率。它还包括减少随机连接的步骤和减少非信息分子(例如未连接末端)的产生的步骤,以提高有效的染色体内读取对的数量。该协议允许获取有关构象结构(例如区室和拓扑关联域)以及高分辨率构象特征(例如DNA环)的信息。

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