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染色质和核纤层蛋白A决定了细胞核的两种不同力学响应机制。

Chromatin and lamin A determine two different mechanical response regimes of the cell nucleus.

作者信息

Stephens Andrew D, Banigan Edward J, Adam Stephen A, Goldman Robert D, Marko John F

机构信息

Department of Molecular Biosciences, Northwestern University, Evanston, IL 60208

Department of Physics and Astronomy, Northwestern University, Evanston, IL 60208.

出版信息

Mol Biol Cell. 2017 Jul 7;28(14):1984-1996. doi: 10.1091/mbc.E16-09-0653. Epub 2017 Jan 5.

Abstract

The cell nucleus must continually resist and respond to intercellular and intracellular mechanical forces to transduce mechanical signals and maintain proper genome organization and expression. Altered nuclear mechanics is associated with many human diseases, including heart disease, progeria, and cancer. Chromatin and nuclear envelope A-type lamin proteins are known to be key nuclear mechanical components perturbed in these diseases, but their distinct mechanical contributions are not known. Here we directly establish the separate roles of chromatin and lamin A/C and show that they determine two distinct mechanical regimes via micromanipulation of single isolated nuclei. Chromatin governs response to small extensions (<3 μm), and euchromatin/heterochromatin levels modulate the stiffness. In contrast, lamin A/C levels control nuclear strain stiffening at large extensions. These results can be understood through simulations of a polymeric shell and cross-linked polymer interior. Our results provide a framework for understanding the differential effects of chromatin and lamin A/C in cell nuclear mechanics and their alterations in disease.

摘要

细胞核必须持续抵抗并响应细胞间和细胞内的机械力,以转导机械信号并维持适当的基因组组织和表达。核力学改变与许多人类疾病相关,包括心脏病、早衰症和癌症。已知染色质和核膜A型核纤层蛋白是这些疾病中受到干扰的关键核机械成分,但其独特的机械作用尚不清楚。在这里,我们直接确定了染色质和核纤层蛋白A/C的不同作用,并表明它们通过对单个分离细胞核的微操作确定了两种不同的力学状态。染色质控制对小延伸(<3μm)的响应,常染色质/异染色质水平调节硬度。相比之下,核纤层蛋白A/C水平在大延伸时控制核应变硬化。这些结果可以通过聚合物壳和交联聚合物内部的模拟来理解。我们的结果为理解染色质和核纤层蛋白A/C在细胞核力学中的不同作用及其在疾病中的改变提供了一个框架。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1ca0/5541848/792e05f2d9b5/1984fig1.jpg

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