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蛋白质电荷阻塞调控的细胞周期特异性相分离。

Cell cycle-specific phase separation regulated by protein charge blockiness.

机构信息

Graduate School of Biostudies, Kyoto University, Kyoto, Japan.

Graduate School of Science, The University of Tokyo, Tokyo, Japan.

出版信息

Nat Cell Biol. 2022 May;24(5):625-632. doi: 10.1038/s41556-022-00903-1. Epub 2022 May 5.

Abstract

Dynamic morphological changes of intracellular organelles are often regulated by protein phosphorylation or dephosphorylation. Phosphorylation modulates stereospecific interactions among structured proteins, but how it controls molecular interactions among unstructured proteins and regulates their macroscopic behaviours remains unknown. Here we determined the cell cycle-specific behaviour of Ki-67, which localizes to the nucleoli during interphase and relocates to the chromosome periphery during mitosis. Mitotic hyperphosphorylation of disordered repeat domains of Ki-67 generates alternating charge blocks in these domains and increases their propensity for liquid-liquid phase separation (LLPS). A phosphomimetic sequence and the sequences with enhanced charge blockiness underwent strong LLPS in vitro and induced chromosome periphery formation in vivo. Conversely, mitotic hyperphosphorylation of NPM1 diminished a charge block and suppressed LLPS, resulting in nucleolar dissolution. Cell cycle-specific phase separation can be modulated via phosphorylation by enhancing or reducing the charge blockiness of disordered regions, rather than by attaching phosphate groups to specific sites.

摘要

细胞内细胞器的动态形态变化通常受到蛋白质磷酸化或去磷酸化的调节。磷酸化调节结构化蛋白质之间的立体特异性相互作用,但它如何控制无结构蛋白质之间的分子相互作用并调节它们的宏观行为尚不清楚。在这里,我们确定了 Ki-67 的细胞周期特异性行为,Ki-67 在间期定位于核仁,在有丝分裂期间重新定位到染色体周围。Ki-67 无规重复结构域的有丝分裂过度磷酸化在这些结构域中产生交替的电荷块,并增加它们发生液-液相分离(LLPS)的倾向。一个磷酸模拟序列和增强的电荷块状的序列在体外经历了强烈的 LLPS,并在体内诱导了染色体周围的形成。相反,NPM1 的有丝分裂过度磷酸化减小了电荷块并抑制了 LLPS,导致核仁溶解。通过增强或减小无序区域的电荷块状,可以调节细胞周期特异性相分离,而不是将磷酸基团附着到特定的位点上。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7229/9106583/5adb1df4ae56/41556_2022_903_Fig1_HTML.jpg

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