细菌
大肠杆菌
生物物理学
共域化
化学
分辨率(逻辑)
生物系统
纳米技术
化学物理
材料科学
生物
生物化学
细胞生物学
计算机科学
人工智能
基因
遗传学
作者
Y Hoang,Christopher A. Azaldegui,Rachel E. Dow,Maria Ghalmi,Julie S. Biteen,Anthony G. Vecchiarelli
标识
DOI:10.1038/s41467-024-47330-4
摘要
Abstract High-resolution imaging of biomolecular condensates in living cells is essential for correlating their properties to those observed through in vitro assays. However, such experiments are limited in bacteria due to resolution limitations. Here we present an experimental framework that probes the formation, reversibility, and dynamics of condensate-forming proteins in Escherichia coli as a means to determine the nature of biomolecular condensates in bacteria. We demonstrate that condensates form after passing a threshold concentration, maintain a soluble fraction, dissolve upon shifts in temperature and concentration, and exhibit dynamics consistent with internal rearrangement and exchange between condensed and soluble fractions. We also discover that an established marker for insoluble protein aggregates, IbpA, has different colocalization patterns with bacterial condensates and aggregates, demonstrating its potential applicability as a reporter to differentiate the two in vivo. Overall, this framework provides a generalizable, accessible, and rigorous set of experiments to probe the nature of biomolecular condensates on the sub-micron scale in bacterial cells.
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