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Bottom-Up Meets Top-Down: The Crossroads of Multiscale Chromatin Modeling

机译:自上而下的符合自上而下:多尺度染色质造型的十字路口

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摘要

Chromatin can be viewed as a hierarchically structured fiber that regulates gene expression. It consists of a complex network of DNA and proteins whose characteristic dynamical modes facilitate compaction and rearrangement in the cell nucleus. These modes stem from chromatin’s fundamental unit, the nucleosome, and their effects are propagated across length scales. Understanding the effects of nucleosome dynamics on the chromatin fiber, primarily through post-translational modifications that occur on the histones, is of central importance to epigenetics. Within the last decade, imaging and chromosome conformation capture techniques have revealed a number of structural and statistical features of the packaged chromatin fiber at a hitherto unavailable level of resolution. Such experiments have led to increased efforts to develop polymer models that aim to reproduce, explain, and predict the contact probability scaling and density heterogeneity. At nanometer scales, available models have focused on the role of the nucleosome and epigenetic marks on local chromatin structure. At micrometer scales, existing models have sought to explain scaling laws and density heterogeneity. Less work, however, has been done to reconcile these two approaches: bottom-up and top-down models of chromatin. In this perspective, we highlight the multiscale simulation models that are driving toward an understanding of chromatin structure and function, from the nanometer to the micron scale, and we highlight areas of opportunity and some of the prospects for new frameworks that bridge these two scales. Taken together, experimental and modeling advances over the last few years have established a robust platform for the study of chromatin fiber structure and dynamics, which will be of considerable use to the chromatin community in developing an understanding of the interplay between epigenomic regulation and molecular structure.
机译:染色质可以被看作是一种调节基因表达的层次结构化纤维。它由DNA和其特性动力模式有利于在细胞核中压实和重排蛋白质的复合物网络。这些模式从染色质的基本单位,核小体干,他们的影响横跨长度尺度传播。了解核小体动力学的影响的染色质纤维,主要是通过在组蛋白中发生的翻译后修饰,是至关重要的,以表观遗传学。在过去的十年中,成像和染色体构象捕获技术已经发现了一些包装染色质纤维的结构和统计特征在分辨率下的迄今不可用水平。这样的实验导致加大了开发力度,旨在重现,解释和预测的接触概率缩放和密度不均匀性聚合物模型。在纳米尺度,可用的模型都集中在当地的染色质结构的核和表观遗传标记的作用。在微米尺度,现有的模式都试图解释标度律和密度不均匀性。更少的工作,但是,已经做了这两种方法调和:染色质的自下而上和自上而下的模式。从这个角度来看,我们强调的是推动朝染色质的结构和功能的理解,从纳米到微米尺度的多尺度模拟模型,我们强调和机会的领域的一些新的框架,桥这两个尺度的前景。总之,实验和建模,在过去几年中的进步已经建立了染色质纤维结构和动力学的研究,这将是相当大的用处,染色质社区开发表观基因调控和分子结构之间的相互作用的理解,一个强大的平台。

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