钙诱导的肌动蛋白解聚降低NMDA通道活性。

Actin filaments are highly concentrated in postsynaptic densities at central excitatory synapses, but their influence on postsynaptic glutamate receptors is unknown. We tested whether actin depolymerization influences NMDA channel activity in whole-cell recording on cultured hippocampal neurons. The ATP- and calcium-dependent rundown of NMDA channels was prevented when actin depolymerization was blocked by phalloidin. Rundown of AMPA/kainate receptors was unaffected by phalloidin. Cytochalasins, which enhance actin-ATP hydrolysis, induced NMDA channel rundown, whereas taxol or colchicine, which stabilize or disrupt microtubule assembly, had no effect. Protease inhibitors also had no effect. Our results suggest that calcium and ATP can influence NMDA channel activity by altering the state of actin polymerization and are consistent with a proposed model in which actin filaments compartmentalize a channel regulatory protein.

肌动蛋白丝在中枢兴奋性突触的突触后致密物中高度富集，但其对突触后谷氨酸受体的影响尚不清楚。我们在培养的海马神经元的全细胞记录中测试了肌动蛋白解聚是否会影响NMDA通道活性。当用鬼笔环肽阻断肌动蛋白解聚时，可防止NMDA通道依赖ATP和钙的功能衰退。AMPA/海人藻酸受体的功能衰退不受鬼笔环肽影响。增强肌动蛋白-ATP水解的细胞松弛素可诱导NMDA通道功能衰退，而稳定或破坏微管组装的紫杉醇或秋水仙碱则无此作用。蛋白酶抑制剂也无作用。我们的结果表明，钙和ATP可通过改变肌动蛋白聚合状态来影响NMDA通道活性，这与肌动蛋白丝分隔通道调节蛋白的模型一致。

Calcium-induced actin depolymerization reduces NMDA channel activity.

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