Structure and assembly of calcium homeostasis modulator proteins

被引:0
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作者
Johanna L. Syrjanen
Kevin Michalski
Tsung-Han Chou
Timothy Grant
Shanlin Rao
Noriko Simorowski
Stephen J. Tucker
Nikolaus Grigorieff
Hiro Furukawa
机构
[1] Cold Spring Harbor Laboratory,WM Keck Structural Biology Laboratory
[2] Howard Hughes Medical Institute,Janelia Research Campus
[3] University of Oxford,Department of Biochemistry
[4] University of Oxford,Clarendon Laboratory, Department of Physics
[5] University of Massachusetts Medical School,RNA Therapeutics Institute
来源
Nature Structural & Molecular Biology | 2020年 / 27卷
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摘要
The biological membranes of many cell types contain large-pore channels through which a wide variety of ions and metabolites permeate. Examples include connexin, innexin and pannexin, which form gap junctions and/or bona fide cell surface channels. The most recently identified large-pore channels are the calcium homeostasis modulators (CALHMs), through which ions and ATP permeate in a voltage-dependent manner to control neuronal excitability, taste signaling and pathologies of depression and Alzheimer’s disease. Despite such critical biological roles, the structures and patterns of their oligomeric assembly remain unclear. Here, we reveal the structures of two CALHMs, chicken CALHM1 and human CALHM2, by single-particle cryo-electron microscopy (cryo-EM), which show novel assembly of the four transmembrane helices into channels of octamers and undecamers, respectively. Furthermore, molecular dynamics simulations suggest that lipids can favorably assemble into a bilayer within the larger CALHM2 pore, but not within CALHM1, demonstrating the potential correlation between pore size, lipid accommodation and channel activity.
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页码:150 / 159
页数:9
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