1. Atomistic Insights of Calmodulin Gating of Complete Ion Channels
- Author
-
Eider Nuñez, Alvaro Villarroel, Arantza Muguruza-Montero, Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), and Eusko Jaurlaritza
- Subjects
calmodulin ,Potassium Channels ,Calmodulin ,Allosteric regulation ,Kv10 ,Kv7 ,Review ,Gating ,Ion Channels ,Catalysis ,Exocytosis ,Calcium in biology ,Inorganic Chemistry ,lcsh:Chemistry ,KCNQ ,Transient Receptor Potential Channels ,Allosteric Regulation ,Protein Domains ,SK2 ,SK4 ,Humans ,M-current ,Calcium Signaling ,Physical and Theoretical Chemistry ,Molecular Biology ,lcsh:QH301-705.5 ,Eag1 ,Spectroscopy ,Ion channel ,Membrane potential ,biology ,Chemistry ,Organic Chemistry ,General Medicine ,Transmembrane protein ,Computer Science Applications ,lcsh:Biology (General) ,lcsh:QD1-999 ,biology.protein ,Biophysics ,TRPV5 ,TRPV6 - Abstract
© 2020 by the authors, Intracellular calcium is essential for many physiological processes, from neuronal signaling and exocytosis to muscle contraction and bone formation. Ca2+ signaling from the extracellular medium depends both on membrane potential, especially controlled by ion channels selective to K+, and direct permeation of this cation through specialized channels. Calmodulin (CaM), through direct binding to these proteins, participates in setting the membrane potential and the overall permeability to Ca2+. Over the past years many structures of complete channels in complex with CaM at near atomic resolution have been resolved. In combination with mutagenesis-function, structural information of individual domains and functional studies, different mechanisms employed by CaM to control channel gating are starting to be understood at atomic detail. Here, new insights regarding four types of tetrameric channels with six transmembrane (6TM) architecture, Eag1, SK2/SK4, TRPV5/TRPV6 and KCNQ1–5, and its regulation by CaM are described structurally. Different CaM regions, N-lobe, C-lobe and EF3/EF4-linker play prominent signaling roles in different complexes, emerging the realization of crucial non-canonical interactions between CaM and its target that are only evidenced in the full-channel structure. Different mechanisms to control gating are used, including direct and indirect mechanical actuation over the pore, allosteric control, indirect effect through lipid binding, as well as direct plugging of the pore. Although each CaM lobe engages through apparently similar alpha-helices, they do so using different docking strategies. We discuss how this allows selective action of drugs with great therapeutic potential., The Government of the Autonomous Community of the Basque Country (IT1165–19) and the Spanish Ministry of Economy, Industry and Competitiveness (RTI2018–097839-B-100) provided financial support for this work. E.N. and A.M-M. were supported by predoctoral contracts of the Basque Government.
- Published
- 2020