Structural basis of antimicrobial membrane coat assembly by human GBP1

被引:0
|
作者
Tanja Kuhm [1 ]
Clémence Taisne [1 ]
Cecilia de Agrela Pinto [1 ]
Luca Gross [2 ]
Evdokia A. Giannopoulou [1 ]
Stefan T. Huber [1 ]
Els Pardon [3 ]
Jan Steyaert [4 ]
Sander J. Tans [3 ]
Arjen J. Jakobi [4 ]
机构
[1] Delft University of Technology,Department of Bionanoscience, Kavli Insitute of Nanoscience
[2] AMOLF,Structural Biology Brussels
[3] VIB-VUB Center for Structural Biology,undefined
[4] Vrije Universiteit Brussel,undefined
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D O I
10.1038/s41594-024-01400-9
中图分类号
学科分类号
摘要
Guanylate-binding proteins (GBPs) are interferon-inducible guanosine triphosphate hydrolases (GTPases) mediating host defense against intracellular pathogens. Their antimicrobial activity hinges on their ability to self-associate and coat pathogen-associated compartments or cytosolic bacteria. Coat formation depends on GTPase activity but how nucleotide binding and hydrolysis prime coat formation remains unclear. Here, we report the cryo-electron microscopy structure of the full-length human GBP1 dimer in its guanine nucleotide-bound state and describe the molecular ultrastructure of the GBP1 coat on liposomes and bacterial lipopolysaccharide membranes. Conformational changes of the middle and GTPase effector domains expose the isoprenylated C terminus for membrane association. The α-helical middle domains form a parallel, crossover arrangement essential for coat formation and position the extended effector domain for intercalation into the lipopolysaccharide layer of gram-negative membranes. Nucleotide binding and hydrolysis create oligomeric scaffolds with contractile abilities that promote membrane extrusion and fragmentation. Our data offer a structural and mechanistic framework for understanding GBP1 effector functions in intracellular immunity.
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页码:172 / 184
页数:12
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