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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Interaction between liprin-alpha and GIT1 is required for AMPA receptor targeting.
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Interaction between liprin-alpha and GIT1 is required for AMPA receptor targeting.

机译:脂蛋白-α和GIT1之间的相互作用是AMPA受体靶向所必需的。

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Liprin-alpha is a multidomain protein that interacts with the LAR family of receptor protein tyrosine phosphatases and the GRIP/ABP family of AMPA receptor-interacting proteins. Previous studies have indicated that liprin-alpha regulates the development of presynaptic active zones and that the association of liprin-alpha with GRIP is required for postsynaptic targeting of AMPA receptors. However, the underlying molecular mechanisms are not well understood. Here we report that liprin-alpha directly interacts with GIT1, a multidomain protein with GTPase-activating protein activity for the ADP-ribosylation factor family of small GTPases known to regulate protein trafficking and the actin cytoskeleton. Electron microscopic analysis indicates that GIT1 distributes to the region of postsynaptic density (PSD) as well as presynaptic active zones. GIT1 is enriched in PSD fractions and forms a complex with liprin-alpha, GRIP, and AMPA receptors in brain. Expression of dominant-negative constructs interfering with the GIT1-liprin-alpha interaction leads to a selective and marked reduction in the dendritic and surface clustering of AMPA receptors in cultured neurons. These results suggest that the GIT1-liprin-alpha interaction is required for AMPA receptor targeting and that GIT1 may play an important role in the organization of presynaptic and postsynaptic multiprotein complexes.
机译:脂蛋白-α是一种多域蛋白,可与受体蛋白酪氨酸磷酸酶的LAR家族和与AMPA受体相互作用的蛋白的GRIP / ABP家族相互作用。先前的研究表明,脂蛋白-α调节突触前活性区的发育,并且脂蛋白-α与GRIP的结合对于AMPA受体的突触后靶向是必需的。但是,潜在的分子机制尚不十分清楚。在这里,我们报道脂蛋白-α与GIT1直接相互作用,GIT1是具有小GTPase的ADP-核糖基化因子家族的GTPase激活蛋白活性的多域蛋白,已知可调节蛋白的运输和肌动蛋白的细胞骨架。电子显微镜分析表明,GIT1分布到突触后密度(PSD)区域以及突触前活动区。 GIT1富含PSD组分,并与脑中的脂蛋白α,GRIP和AMPA受体形成复合物。显性阴性构建体的表达干扰了GIT1-liprin-α相互作用,导致培养的神经元中AMPA受体的树突状和表面聚集选择性和显着降低。这些结果表明,AMPA受体靶向需要GIT1-liprin-alpha相互作用,并且GIT1在突触前和突触后多蛋白复合物的组织中可能发挥重要作用。

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