| Literature DB >> 30523075 |
Begoña Monterroso1, Silvia Zorrilla1, Marta Sobrinos-Sanguino2, Miguel A Robles-Ramos2, Marina López-Álvarez2, William Margolin3, Christine D Keating4, Germán Rivas1.
Abstract
Macromolecular condensation resulting from biologically regulated liquid-liquid phase separation is emerging as a mechanism to organize intracellular space in eukaryotes, with broad implications for cell physiology and pathology. Despite their small size, bacterial cells are also organized by proteins such as FtsZ, a tubulin homolog that assembles into a ring structure precisely at the cell midpoint and is required for cytokinesis. Here, we demonstrate that FtsZ can form crowding-induced condensates, reminiscent of those observed for eukaryotic proteins. Formation of these FtsZ-rich droplets occurs when FtsZ is bound to SlmA, a spatial regulator of FtsZ that antagonizes polymerization, while also binding to specific sites on chromosomal DNA. The resulting condensates are dynamic, allowing FtsZ to undergo GTP-driven assembly to form protein fibers. They are sensitive to compartmentalization and to the presence of a membrane boundary in cell mimetic systems. This is a novel example of a bacterial nucleoprotein complex exhibiting condensation into liquid droplets, suggesting that phase separation may also play a functional role in the spatiotemporal organization of essential bacterial processes.Entities:
Keywords: bacterial division; biomolecular condensation; droplet microfluidics; macromolecular crowding; phase separation
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Year: 2018 PMID: 30523075 PMCID: PMC6322363 DOI: 10.15252/embr.201845946
Source DB: PubMed Journal: EMBO Rep ISSN: 1469-221X Impact factor: 8.807