期刊
SCIENCE
卷 330, 期 6000, 页码 105-109出版社
AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/science.1191086
关键词
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资金
- NIH [HL55426, AI058173]
- Novartis Institutes for Biomedical Research
- American Heart Association
- NSFC [30871011]
- Tianjin S&T Support Project [08ZCKFSH04500]
- 973 program [2010CB945001]
Calcium signals, pivotal in controlling cell function, can be generated by calcium entry channels activated by plasma membrane depolarization or depletion of internal calcium stores. We reveal a regulatory link between these two channel subtypes mediated by the ubiquitous calcium-sensing STIM proteins. STIM1 activation by store depletion or mutational modification strongly suppresses voltage-operated calcium (Ca(V)1.2) channels while activating store-operated Orai channels. Both actions are mediated by the short STIM-Orai activating region (SOAR) of STIM1. STIM1 interacts with Ca(V)1.2 channels and localizes within discrete endoplasmic reticulum/plasma membrane junctions containing both Ca(V)1.2 and Orai1 channels. Hence, STIM1 interacts with and reciprocally controls two major calcium channels hitherto thought to operate independently. Such coordinated control of the widely expressed Ca(V)1.2 and Orai channels has major implications for Ca2+ signal generation in excitable and nonexcitable cells.
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