Ion currents through the voltage sensor domain of distinct families of proteins.

J Biol Phys

Departamento de Genética del Desarrollo y Fisiología Molecular, Instituto de Biotecnología, Universidad Nacional Autónoma de México, Cuernavaca, Morelos, 62210, Mexico.

Published: December 2023

AI Article Synopsis

  • The membrane potential (V) influences various physiological activities, and the voltage sensor domain (VSD) is key in enabling voltage sensitivity in proteins like ion channels and exchangers.
  • VSDs consist of four transmembrane segments (S1-S4) with essential positive amino acids in S4 that respond to voltage changes by moving along the membrane without generating ionic currents.
  • Gating pore currents may arise from certain VSDs, often due to a lack of conserved positives in S4, and can be classified into pathological, physiological, and artificial types, with S4 positioning determining their voltage dependency across protein families.

Article Abstract

The membrane potential of a cell (V) regulates several physiological processes. The voltage sensor domain (VSD) is a region that confers voltage sensitivity to different types of transmembrane proteins such as the following: voltage-gated ion channels, the voltage-sensing phosphatase (Ci-VSP), and the sperm-specific Na/H exchanger (sNHE). VSDs contain four transmembrane segments (S1-S4) and several positively charged amino acids in S4, which are essential for the voltage sensitivity of the protein. Generally, in response to changes of the V, the positive residues of S4 displace along the plasma membrane without generating ionic currents through this domain. However, some native (e.g., Hv1 channel) and mutants of VSDs produce ionic currents. These gating pore currents are usually observed in VSDs that lack one or more of the conserved positively charged amino acids in S4. The gating pore currents can also be induced by the isolation of a VSD from the rest of the protein domains. In this review, we summarize gating pore currents from all families of proteins with VSDs with classification into three cases: (1) pathological, (2) physiological, and (3) artificial currents. We reinforce the model in which the position of S4 that lacks the positively charged amino acid determines the voltage dependency of the gating pore current of all VSDs independent of protein families.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10651576PMC
http://dx.doi.org/10.1007/s10867-023-09645-zDOI Listing

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