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Evaluation and comparison of methods for recapitulation of 3D spatial chromatin structures

机译:3D空间染色质结构携带方法的评价与比较

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摘要

How chromosomes fold and how distal genomic elements interact with one another at a genomic scale have been actively pursued in the past decade following the seminal work describing the Chromosome Conformation Capture (3C) assay. Essentially, 3C-based technologies produce two-dimensional (2D) contact maps that capture interactions between genomic fragments. Accordingly, a plethora of analytical methods have been proposed to take a 2D contact map as input to recapitulate the underlying whole genome three-dimensional (3D) structure of the chromatin. However, their performance in terms of several factors, including data resolution and ability to handle contact map features, have not been sufficiently evaluated. This task is taken up in this article, in which we consider several recent and/or well-regarded methods, both optimizationbased and model-based, for their aptness of producing 3D structures using contact maps generated based on a population of cells. These methods are evaluated and compared using both simulated and real data. Several criteria have been used. For simulated data sets, the focus is on accurate recapitulation of the entire structure given the existence of the gold standard. For real data sets, comparison with distances measured by Florescence in situ Hybridization and consistency with several genomic features of known biological functions are examined.
机译:染色体如何折叠以及远端基因组元素在过去十年中,在描述染色体构象捕获(3C)测定的精髓工作之后,在过去十年中已经积极地追求了基因组规模的彼此相互作用。基本上,基于3C的技术产生二维(2D)联系地图,该映射捕获基因组片段之间的相互作用。因此,已经提出了一种分析方法,以将2D接触图作为输入,以概括染色质的底层全基因组三维(3D)结构。但是,它们在几种因素方面的性能,包括数据分辨率和处理联系地图特征的能力,没有得到足够的评估。本文占据了这项任务,其中我们考虑了几种最近和/或良好的方法,包括基于优化和模型的模型,用于使用基于细胞群生成的联系地图产生3D结构。使用模拟和实际数据进行评估和比较这些方法。已经使用了几个标准。对于模拟数据集,鉴于金标准的存在,重点是对整个结构的准确速度。对于真实数据集,研究了通过繁殖的距离测量的比较原位杂交和与已知生物学功能的若干基因组特征的一致性。

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