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- W3133807592 abstract "FtsZ is an essential and central protein for cell division in most bacteria. Because of its ability to organize into dynamic polymers at the cell membrane and recruit other protein partners to form a “divisome”, FtsZ is a leading target in the quest for new antibacterial compounds. Strategies to potentially arrest the essential and tightly regulated cell division process include perturbing FtsZ’s ability to interact with itself and other divisome proteins. Here, we discuss the available methodologies to screen for and characterize those interactions. In addition to assays that measure protein-ligand interactions in solution, we also discuss the use of minimal membrane systems and cell-like compartments to better approximate the native bacterial cell environment and hence provide a more accurate assessment of a candidate compound’s potential in vivo effect. We particularly focus on ways to measure and inhibit under-explored interactions between FtsZ and partner proteins. Finally, we discuss recent evidence that FtsZ forms biomolecular condensates in vitro, and the potential implications of these assemblies in bacterial resistance to antibiotic treatment." @default.
- W3133807592 created "2021-03-15" @default.
- W3133807592 creator A5011693234 @default.
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- W3133807592 creator A5056661498 @default.
- W3133807592 creator A5058194019 @default.
- W3133807592 creator A5063363413 @default.
- W3133807592 date "2021-03-04" @default.
- W3133807592 modified "2023-09-27" @default.
- W3133807592 title "FtsZ Interactions and Biomolecular Condensates as Potential Targets for New Antibiotics" @default.
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