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Zinc inhibition of monomeric and dimeric proton channels suggests cooperative gating
Author(s) -
Musset Boris,
Smith Susan M. E.,
Rajan Sindhu,
Cherny Vladimir V.,
Sujai Sukrutha,
Morgan Deri,
DeCoursey Thomas E.
Publication year - 2010
Publication title -
the journal of physiology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.802
H-Index - 240
eISSN - 1469-7793
pISSN - 0022-3751
DOI - 10.1113/jphysiol.2010.188318
Subject(s) - gating , chemistry , biophysics , zinc , proton , monomer , biology , physics , organic chemistry , quantum mechanics , polymer
Voltage‐gated proton channels are strongly inhibited by Zn 2+ , which binds to His residues. However, in a molecular model, the two externally accessible His are too far apart to coordinate Zn 2+ . We hypothesize that high‐affinity Zn 2+ binding occurs at the dimer interface between pairs of His residues from both monomers. Consistent with this idea, Zn 2+ effects were weaker in monomeric channels. Mutation of His 193 and His 140 in various combinations and in tandem dimers revealed that channel opening was slowed by Zn 2+ only when at least one His was present in each monomer, suggesting that in wild‐type (WT) H V 1, Zn 2+ binding between His of both monomers inhibits channel opening. In addition, monomeric channels opened exponentially, and dimeric channels opened sigmoidally. Monomeric channel gating had weaker temperature dependence than dimeric channels. Finally, monomeric channels opened 6.6 times faster than dimeric channels. Together, these observations suggest that in the proton channel dimer, the two monomers are closely apposed and interact during a cooperative gating process. Zn 2+ appears to slow opening by preventing movement of the monomers relative to each other that is prerequisite to opening. These data also suggest that the association of the monomers is tenuous and allows substantial freedom of movement. The data support the idea that native proton channels are dimeric. Finally, the idea that monomer–dimer interconversion occurs during activation of phagocytes appears to be ruled out.

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