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糖原相分离驱动大分子重排和不对称分裂。 (你提供的原文似乎不完整,句末缺少具体细胞类型等相关信息)

Glycogen phase separation drives macromolecular rearrangement and asymmetric division in .

作者信息

Thappeta Yashna, Cañas-Duarte Silvia J, Kallem Till, Fragasso Alessio, Xiang Yingjie, Gray William, Lee Cheyenne, Cegelski Lynette, Jacobs-Wagner Christine

机构信息

Sarafan Chemistry, Engineering, and Medicine for Human Health Institute, Stanford University, Stanford, CA, USA.

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

出版信息

bioRxiv. 2024 Apr 20:2024.04.19.590186. doi: 10.1101/2024.04.19.590186.

Abstract

Bacteria often experience nutrient limitation in nature and the laboratory. While exponential and stationary growth phases are well characterized in the model bacterium , little is known about what transpires inside individual cells during the transition between these two phases. Through quantitative cell imaging, we found that the position of nucleoids and cell division sites becomes increasingly asymmetric during transition phase. These asymmetries were coupled with spatial reorganization of proteins, ribosomes, and RNAs to nucleoid-centric localizations. Results from live-cell imaging experiments, complemented with genetic and C whole-cell nuclear magnetic resonance spectroscopy studies, show that preferential accumulation of the storage polymer glycogen at the old cell pole leads to the observed rearrangements and asymmetric divisions. In vitro experiments suggest that these phenotypes are likely due to the propensity of glycogen to phase separate in crowded environments, as glycogen condensates exclude fluorescent proteins under physiological crowding conditions. Glycogen-associated differences in cell sizes between strains and future daughter cells suggest that glycogen phase separation allows cells to store large glucose reserves without counting them as cytoplasmic space.

摘要

在自然环境和实验室中,细菌常常会经历营养限制。虽然模式细菌的指数生长期和稳定期已得到充分表征,但对于这两个阶段之间的转变过程中单个细胞内部发生了什么却知之甚少。通过定量细胞成像,我们发现类核和细胞分裂位点的位置在转变期变得越来越不对称。这些不对称性与蛋白质、核糖体和RNA向以类核为中心的定位的空间重组相关联。活细胞成像实验的结果,辅以遗传学和全细胞核磁共振光谱研究,表明储存聚合物糖原在旧细胞极的优先积累导致了观察到的重排和不对称分裂。体外实验表明,这些表型可能是由于糖原在拥挤环境中发生相分离的倾向,因为在生理拥挤条件下糖原凝聚物会排斥荧光蛋白。菌株与未来子细胞之间与糖原相关的细胞大小差异表明,糖原相分离使细胞能够储存大量葡萄糖储备而不将其计入细胞质空间。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2e13/11042326/5942533215d4/nihpp-2024.04.19.590186v1-f0001.jpg

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