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Dynamics of Chromatin Decondensation Reveals the Structural Integrity of a Mechanically Prestressed Nucleus

机译:染色质解聚动力学揭示了机械预应力核的结构完整性。

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摘要

Genome organization within the cell nucleus is a result of chromatin condensation achieved by histone tail-tail interactions and other nuclear proteins that counter the outward entropic pressure of the polymeric DNA. We probed the entropic swelling of chromatin driven by enzymatic disruption of these interactions in isolated mammalian cell nuclei. The large-scale decondensation of chromatin and the eventual rupture of the nuclear membrane and lamin network due to this entropic pressure were observed by fluorescence imaging. This swelling was accompanied by nuclear softening, an effect that we quantified by measuring the fluctuations of an optically trapped bead adhered onto the nucleus. We also measured the pressure at which the nuclear scaffold ruptured using an atomic force microscope cantilever. A simple theory based on a balance of forces in a swelling porous gel quantitatively explains the diffusive dynamics of swelling. Our experiments on decondensation of chromatin in nuclei suggest that its compaction is a critical parameter in controlling nuclear stability.
机译:细胞核内的基因组组织是染色质凝结的结果,染色质凝结是通过组蛋白尾巴相互作用和其他抵消聚合DNA向外熵压力的核蛋白实现的。我们探讨了由孤立的哺乳动物细胞核中这些相互作用的酶促破坏驱动的染色质的熵膨胀。通过荧光成像观察到染色质的大规模缩聚以及由于这种熵压而导致的核膜和层状网络的最终破裂。这种肿胀伴随着核软化,我们通过测量粘附在核上的光学捕获的微珠的波动来量化这种效应。我们还使用原子力显微镜悬臂梁测量了核支架破裂的压力。基于溶胀多孔凝胶中力平衡的简单理论定量地解释了溶胀的扩散动力学。我们对核中染色质的缩合实验表明,其紧实度是控制核稳定性的关键参数。

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