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Challenges for visualizing three‐dimensional data in genomic browsers

机译:在基因组浏览器中可视化三维数据的挑战

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摘要

Genomic interactions reveal the spatial organization of genomes and genomic domains, which is known to play key roles in cell function. Physical proximity can be represented as two‐dimensional heat maps or matrices. From these, three‐dimensional (3D) conformations of chromatin can be computed revealing coherent structures that highlight the importance of nonsequential relationships across genomic features. Mainstream genomic browsers have been classically developed to display compact, stacked tracks based on a linear, sequential, per‐chromosome coordinate system. Genome‐wide comparative analysis demands new approaches to data access and new layouts for analysis. The legibility can be compromised when displaying track‐aligned second dimension matrices, which require greater screen space. Moreover, 3D representations of genomes defy vertical alignment in track‐based genome browsers. Furthermore, investigation at previously unattainable levels of detail is revealing multiscale, multistate, time‐dependent complexity. This article outlines how these challenges are currently handled in mainstream browsers as well as how novel techniques in visualization are being explored to address them. A set of requirements for coherent visualization of novel spatial genomic data is defined and the resulting potential for whole genome visualization is described.
机译:基因组相互作用揭示了基因组和基因组域的空间组织,已知在细胞功能中起关键作用。物理接近度可以表示为二维热图或矩阵。通过这些,可以计算出染色质的三维(3D)构象,揭示了相干的结构,这些结构突出了跨基因组特征的非顺序关系的重要性。主流基因组浏览器经过经典开发,可以显示基于线性,顺序,每个染色体坐标系的紧凑,堆叠的轨道。全基因组比较分析需要新的数据访问方法和新的分析布局。当显示需要更大屏幕空间的,按轨迹对齐的第二维矩阵时,可读性可能会受到影响。此外,基因组的3D表示法无法在基于轨道的基因组浏览器中进行垂直对齐。此外,对以前无法达到的详细程度的研究揭示了多尺度,多状态,时间依赖性的复杂性。本文概述了当前在主流浏览器中如何应对这些挑战,以及如何探索可视化中的新颖技术来解决这些挑战。定义了一套新颖的空间基因组数据的相干可视化要求,并描述了全基因组可视化的潜在潜力。

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