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Chromatin conformation analysis of primary patient tissue using a low input Hi-C method

机译:使用低输入Hi-C方法对主要患者组织进行染色质构象分析

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Chromatin conformation constitutes a fundamental level of eukaryotic genome regulation. However, our ability to examine its biological function and role in disease is limited by the large amounts of starting material required to perform current experimental approaches. Here, we present Low-C, a Hi-C method for low amounts of input material. By systematically comparing Hi-C libraries made with decreasing amounts of starting material we show that Low-C is highly reproducible and robust to experimental noise. To demonstrate the suitability of Low-C to analyse rare cell populations, we produce Low-C maps from primary B-cells of a diffuse large B-cell lymphoma patient. We detect a common reciprocal translocation t(3;14)(q27;q32) affecting the BCL6 and IGH loci and abundant local structural variation between the patient and healthy B-cells. The ability to study chromatin conformation in primary tissue will be fundamental to fully understand the molecular pathogenesis of diseases and to eventually guide personalised therapeutic strategies.
机译:染色质构象构成了真核基因组调控的基本水平。但是,我们检查其生物学功能和在疾病中的作用的能力受到执行当前实验方法所需的大量起始材料的限制。在这里,我们介绍了Low-C,一种用于少量输入材料的Hi-C方法。通过系统地比较使用减少的起始原料制成的Hi-C库,我们显示出Low-C具有很高的重现性,并且对实验噪声具有鲁棒性。为了证明Low-C分析稀有细胞群的适用性,我们从一名弥漫性大B细胞淋巴瘤患者的原代B细胞中产生了Low-C图。我们检测到一个常见的相互易位t(3; 14)(q27; q32)影响BCL6和IGH基因座以及患者和健康B细胞之间丰富的局部结构变异。研究原发组织中染色质构象的能力将是全面了解疾病的分子发病机制并最终指导个性化治疗策略的基础。

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