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钙杆菌染色体在体内的构象与模型对细胞样限制中超螺旋聚合物的预测相匹配。

Caulobacter chromosome in vivo configuration matches model predictions for a supercoiled polymer in a cell-like confinement.

机构信息

Department of Developmental Biology, Stanford University, Stanford, CA 94305, USA.

出版信息

Proc Natl Acad Sci U S A. 2013 Jan 29;110(5):1674-9. doi: 10.1073/pnas.1220824110. Epub 2013 Jan 14.

Abstract

We measured the distance between fluorescent-labeled DNA loci of various interloci contour lengths in Caulobacter crescentus swarmer cells to determine the in vivo configuration of the chromosome. For DNA segments less than about 300 kb, the mean interloci distances, , scale as n(0.22), where n is the contour length, and cell-to-cell distribution of the interloci distance r is a universal function of r/n(0.22) with broad cell-to-cell variability. For DNA segments greater than about 300 kb, the mean interloci distances scale as n, in agreement with previous observations. The 0.22 value of the scaling exponent for short DNA segments is consistent with theoretical predictions for a branched DNA polymer structure. Predictions from Brownian dynamics simulations of the packing of supercoiled DNA polymers in an elongated cell-like confinement are also consistent with a branched DNA structure, and simulated interloci distance distributions predict that confinement leads to "freezing" of the supercoiled configuration. Lateral positions of labeled loci at comparable positions along the length of the cell are strongly correlated when the longitudinal locus positions differ by <0.16 μm. We conclude that the chromosome structure is supercoiled locally and elongated at large length scales and that substantial cell-to-cell variability in the interloci distances indicates that in vivo crowding prevents the chromosome from reaching an equilibrium arrangement. We suggest that the force causing rapid transport of loci remote from the parS centromere to the distal cell pole may arise from the release at the polar region of potential energy within the supercoiled DNA.

摘要

我们测量了各种不同染色体轮廓长度的 DNA 基因座之间的荧光标记基因座之间的距离,以确定活体内染色体的结构。对于小于约 300kb 的 DNA 片段,平均基因座间距离 与 n(0.22)成正比,其中 n 是染色体轮廓长度,基因座间距离 r 的细胞间分布是 r/n(0.22)的通用函数,细胞间变异性较大。对于大于约 300kb 的 DNA 片段,平均基因座间距离与 n 成正比,这与以前的观察结果一致。短 DNA 片段的标度指数 0.22 值与支化 DNA 聚合物结构的理论预测一致。在长形细胞状限制下对超螺旋 DNA 聚合物包装的布朗动力学模拟的预测也与支化 DNA 结构一致,模拟的基因座间距离分布预测限制导致超螺旋构象的“冻结”。当纵向基因座位置相差 <0.16μm 时,在细胞长度上可比位置处标记基因座的横向位置高度相关。我们得出结论,染色体结构在局部超螺旋化,在大尺度上伸长,并且基因座间距离的大量细胞间变异性表明,活体内拥挤阻止了染色体达到平衡排列。我们建议,导致远离 parS 着丝粒的基因座快速运送到远端细胞极的力可能来自超螺旋 DNA 中在极区释放的势能。

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本文引用的文献

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