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The molecular basis for T-type Ca2+ channel inhibition by G protein beta2gamma2 subunits.


ABSTRACT: Gbetagamma, a ubiquitous second messenger, relays external signals from G protein-coupled receptors to networks of intracellular effectors, including voltage-dependent calcium channels. Unlike high-voltage-activated Ca(2+) channels, the inhibition of low-voltage-activated Ca(2+) channels is subtype-dependent and mediated selectively by Gbeta(2)-containing dimers. Yet, the molecular basis for this exquisite selectivity remains unknown. Here, we used pure recombinant Gbetagamma subunits to establish that the Gbeta(2)gamma(2) dimer can selectively reconstitute the inhibition of alpha(1H) channels in isolated membrane patches. This inhibition is the result of a reduction in channel open probability that is not accompanied by a change in channel expression or an alteration in active-channel gating. By exchanging residues between the active Gbeta(2) subunit and the inactive Gbeta(1) subunit, we identified a cluster of amino acids that functionally distinguish Gbeta(2) from other Gbeta subunits. These amino acids on the beta-torus identify a region that is distinct from those regions that contact the Galpha subunit or other effectors.

SUBMITTER: DePuy SD 

PROVIDER: S-EPMC1600004 | biostudies-literature | 2006 Sep

REPOSITORIES: biostudies-literature

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The molecular basis for T-type Ca2+ channel inhibition by G protein beta2gamma2 subunits.

DePuy Seth D SD   Yao Junlan J   Hu Changlong C   McIntire William W   Bidaud Isabelle I   Lory Philippe P   Rastinejad Fraydoon F   Gonzalez Carlos C   Garrison James C JC   Barrett Paula Q PQ  

Proceedings of the National Academy of Sciences of the United States of America 20060914 39


Gbetagamma, a ubiquitous second messenger, relays external signals from G protein-coupled receptors to networks of intracellular effectors, including voltage-dependent calcium channels. Unlike high-voltage-activated Ca(2+) channels, the inhibition of low-voltage-activated Ca(2+) channels is subtype-dependent and mediated selectively by Gbeta(2)-containing dimers. Yet, the molecular basis for this exquisite selectivity remains unknown. Here, we used pure recombinant Gbetagamma subunits to establi  ...[more]

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