4.8 Article

Cyclodextrins increase membrane tension and are universal activators of mechanosensitive channels

出版社

NATL ACAD SCIENCES
DOI: 10.1073/pnas.2104820118

关键词

methyl-beta-cyclodextrin; phospholipids; cryo-electron microscopy; patch clamp

资金

  1. National Health and Medical Research Council of Australia Principal Research Fellowship [APP1135974]
  2. New South Wales Health Early-Mid Career Research Fellowship

向作者/读者索取更多资源

Research demonstrates that cyclodextrins can mimic membrane tension and activate the bacterial MscS channel, but a specific amount of cyclodextrins is needed for channel gating. However, cholesterol-loaded CDs do not activate the MscS channel. CD-mediated lipid removal causes desensitization of the MscS channel, depending on the lipid environment.
The bacterial mechanosensitive channel of small conductance (MscS) has been extensively studied to understand how mechanical forces are converted into the conformational changes that underlie mechanosensitive (MS) channel gating. We showed that lipid removal by p-cyclodextrin can mimic membrane tension. Here, we show that all cyclodextrins (CDs) can activate reconstituted Escherichia coli MscS, that MscS activation by CDs depends on CD-mediated lipid removal, and that the CD amount required to gate MscS scales with the channel's sensitivity to membrane tension. Importantly, cholesterol-loaded CDs do not activate MscS. CD-mediated lipid removal ultimately causes MscS desensitization, which we show is affected by the lipid environment. While many MS channels respond to membrane forces, generalized by the force-from-lipids principle, their different molecular architectures suggest that they use unique ways to convert mechanical forces into conformational changes. To test whether CDs can also be used to activate other MS channels, we chose to investigate the mechanosensitive channel of large conductance (MscL) and demonstrate that CDs can also activate this structurally unrelated channel. Since CDs can open the least tension-sensitive MS channel, MscL, they should be able to open any MS channel that responds to membrane tension. Thus, CDs emerge as a universal tool for the structural and functional characterization of unrelated MS channels.

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