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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >PICK1 targets activated protein kinase Calpha to AMPA receptor clusters in spines of hippocampal neurons and reduces surface levels of the AMPA-type glutamate receptor subunit 2.
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PICK1 targets activated protein kinase Calpha to AMPA receptor clusters in spines of hippocampal neurons and reduces surface levels of the AMPA-type glutamate receptor subunit 2.

机译:PICK1将活化的蛋白激酶Calpha靶向海马神经元棘中的AMPA受体簇,并降低AMPA型谷氨酸受体亚基2的表面水平。

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摘要

The PICK1 protein interacts in neurons with the AMPA-type glutamate receptor subunit 2 (GluR2) and with several other membrane receptors via its single PDZ domain. We show that PICK1 also binds in neurons and in heterologous cells to protein kinase Calpha (PKCalpha) and that the interaction is highly dependent on the activation of the kinase. The formation of PICK1-PKCalpha complexes is strongly induced by TPA, and PICK1-PKCalpha complexes are cotargeted with PICK1-GluR2 complexes to spines, where GluR2 is found to be phosphorylated by PKC on serine 880. PICK1 also reduces the plasma membrane levels of the GluR2 subunit, consistent with a targeting function of PICK1 and a PKC-facilitated release of GluR2 from the synaptic anchoring proteins ABP and GRIP. This work indicates that PICK1 functions as a targeting and transport protein that directs the activated form of PKCalpha to GluR2 in spines, leading to the activity-dependent release of GluR2 from synaptic anchor proteins and the PICK1-dependent transport of GluR2 from the synaptic membrane.
机译:PICK1蛋白在神经元中与AMPA型谷氨酸受体亚基2(GluR2)以及其他几个膜受体通过其单个PDZ域相互作用。我们显示,PICK1还在神经元和异源细胞中结合蛋白激酶Calpha(PKCalpha),并且相互作用高度依赖于激酶的激活。 TPA强烈诱导PICK1-PKCalpha复合物的形成,并且PICK1-PKCalpha复合物与PICK1-GluR2复合物共同靶向到棘突,在其中发现GluR2被PKC在丝氨酸880上磷酸化。PICK1还降低了其浆膜的水平。 GluR2亚基,与PICK1的靶向功能和PKC促进GluR2从突触锚定蛋白ABP和GRIP的释放一致。这项工作表明,PICK1充当靶向和转运蛋白,将激活形式的PKCalpha引导到棘突中的GluR2,从而导致GluR2从突触锚蛋白中的活性依赖性释放以及GluR2从突触膜的PICK1依赖性转运。

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