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Histidine168 is crucial for ΔpH-dependent gating of the human voltage-gated proton channel, hHV1

Authors :
Sarah Thomas
Vladimir V. Cherny
Susan M.E. Smith
Thomas E. DeCoursey
Deri Morgan
Source :
The Journal of General Physiology
Publication Year :
2018
Publisher :
Rockefeller University Press, 2018.

Abstract

Voltage-gated proton channels open appropriately in myriad physiological situations because their gating is powerfully modulated by both pHo and pHi. Cherny et al. serendipitously identify a histidine at the inner end of the S3 helix that is required for the response to pHi.<br />We recently identified a voltage-gated proton channel gene in the snail Helisoma trivolvis, HtHV1, and determined its electrophysiological properties. Consistent with early studies of proton currents in snail neurons, HtHV1 opens rapidly, but it unexpectedly exhibits uniquely defective sensitivity to intracellular pH (pHi). The H+ conductance (gH)-V relationship in the voltage-gated proton channel (HV1) from other species shifts 40 mV when either pHi or pHo (extracellular pH) is changed by 1 unit. This property, called ΔpH-dependent gating, is crucial to the functions of HV1 in many species and in numerous human tissues. The HtHV1 channel exhibits normal pHo dependence but anomalously weak pHi dependence. In this study, we show that a single point mutation in human hHV1—changing His168 to Gln168, the corresponding residue in HtHV1—compromises the pHi dependence of gating in the human channel so that it recapitulates the HtHV1 response. This location was previously identified as a contributor to the rapid gating kinetics of HV1 in Strongylocentrotus purpuratus. His168 mutation in human HV1 accelerates activation but accounts for only a fraction of the species difference. H168Q, H168S, or H168T mutants exhibit normal pHo dependence, but changing pHi shifts the gH-V relationship on average by

Details

Language :
English
ISSN :
15407748 and 00221295
Volume :
150
Issue :
6
Database :
OpenAIRE
Journal :
The Journal of General Physiology
Accession number :
edsair.doi.dedup.....7a9acab9f71d66400b45ec8394ba91b2