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DNA 含量有助于控制 的核大小。

DNA content contributes to nuclear size control in .

机构信息

Evolutionary Cell Biology Laboratory, Faculty of Science, Yamaguchi University, Yoshida 1677-1, Yamaguchi City, 753-8512, Japan.

Laboratory of Molecular Developmental Biology, Department of Biology, Graduate School of Sciences and Technology for Innovation, Yamaguchi University, Yoshida 1677-1, Yamaguchi City, 753-8512, Japan.

出版信息

Mol Biol Cell. 2020 Nov 15;31(24):2703-2717. doi: 10.1091/mbc.E20-02-0113. Epub 2020 Sep 30.

Abstract

Cells adapt to drastic changes in genome quantity during evolution and cell division by adjusting the nuclear size to exert genomic functions. However, the mechanism by which DNA content within the nucleus contributes to controlling the nuclear size remains unclear. Here, we experimentally evaluated the effects of DNA content by utilizing cell-free egg extracts and imaging of in vivo embryos. Upon manipulation of DNA content while maintaining cytoplasmic effects constant, both plateau size and expansion speed of the nucleus correlated highly with DNA content. We also found that nuclear expansion dynamics was altered when chromatin interaction with the nuclear envelope or chromatin condensation was manipulated while maintaining DNA content constant. Furthermore, excess membrane accumulated on the nuclear surface when the DNA content was low. These results clearly demonstrate that nuclear expansion is determined not only by cytoplasmic membrane supply but also by the physical properties of chromatin, including DNA quantity and chromatin structure within the nucleus, rather than the coding sequences themselves. In controlling the dynamics of nuclear expansion, we propose that chromatin interaction with the nuclear envelope plays a role in transmitting chromatin repulsion forces to the nuclear membrane.

摘要

细胞通过调整核大小来发挥基因组功能,从而适应进化和细胞分裂过程中基因组数量的剧烈变化。然而,细胞核内的 DNA 含量如何控制核大小的机制尚不清楚。在这里,我们通过利用无细胞卵提取物和体内胚胎成像来实验评估 DNA 含量的影响。在维持细胞质效应不变的情况下,对 DNA 含量进行操作,核的平台大小和扩张速度与 DNA 含量高度相关。我们还发现,当维持 DNA 含量不变而改变核膜与染色质相互作用或染色质浓缩时,核扩张动力学会发生改变。此外,当 DNA 含量较低时,核表面会积累多余的膜。这些结果清楚地表明,核扩张不仅由细胞质膜供应决定,还由细胞核内染色质的物理性质决定,包括 DNA 数量和染色质结构,而不是编码序列本身。在控制核扩张动力学方面,我们提出染色质与核膜的相互作用在将染色质排斥力传递到核膜中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4b86/7927187/5bcfb4cd0516/mbc-31-2703-g001.jpg

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