Interaction of SNARE complexes with P/Q-type calcium channels in rat cerebellar synaptosomes

被引:114
作者
MartinMoutot, N
Charvin, N
Leveque, C
Sato, K
Nishiki, T
Kozaki, S
Takahashi, M
Seagar, M
机构
[1] MITSUBISHI KASEI INST LIFE SCI,MACHIDA,TOKYO 194,JAPAN
[2] UNIV OSAKA PREFECTURE,DEPT VET SCI,OSAKA 593,JAPAN
关键词
D O I
10.1074/jbc.271.12.6567
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
P- and Q-type calcium channels, which trigger rapid neurotransmitter release at many mammalian synapses, are blocked by omega-conotoxin MVIIC. I-125-omega Conotoxin MVIIC binding to rat cerebellar synaptosomes was not displaced by omega-conotogins GVIA or MVIIA (K-i > 1 mu M), which are selective for N-type calcium channels. Solubilized I-125-omega-conotoxin MMIC receptors were specifically recognized by antibodies directed against alpha(1)A calcium channel subunits, proteins known to constitute a pore with P/Q-like channel properties, Antibodies against syntaxin 1, SNAP 25, and VAMP 2 (synaptobrevin) each immunoprecipitated a similar fraction (20-40%) of omega-conotoxin MVIIC receptors. Immunoprecipitation was not additive, suggesting that heterotrimeric (SNARE) complexes containing these three proteins interact with P/Q-type calcium channels. Immobilized monoclonal anti-syntaxin antibodies retained ru,A calcium channel subunits of 220, 180 and 160 kDa monitored by immunoblotting with site directed antibodies. Synaptotagmin was detected in channel-associated complexes; but not synaptophysin, Rab 3A nor rat cysteine string protein, Trimeric SNARE complexes are implicated in calcium-dependent exocytosis, a process thought to be regulated by synaptotagmin. Our results indicate that these proteins interact with P/Q-type calcium channels, which may optimize their location within domains of calcium influx.
引用
收藏
页码:6567 / 6570
页数:4
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