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Distinct LIN-10 domains are required for its neuronal function, its epithelial function, and its synaptic localization

机译:神经元功能,上皮功能和突触定位需要不同的LIN-10结构域

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alpha-Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid (AMPA)-type glutamate receptors (AMPARs) mediate excitatory neurotransmission at neuronal synapses, and their regulated localization plays a role in synaptic plasticity. In Caenorhabditis elegans, the PDZ and PTB domain-containing protein LIN-10 is required both for the synaptic localization of the AMPAR subunit GLR-1 and for vulval fate induction in epithelia. Here, we examine the role that different LIN-10 domains play in GLR-1 localization. We find that an amino-terminal region of LIN-10 directs LIN-10 protein localization to the Golgi and to synaptic clusters. In addition, mutations in the carboxyl-terminal PDZ domains prevent LIN-10 from regulating GLR-1 localization in neurons but do not prevent LIN-10 from functioning in the vulval epithelia. A mutation in the amino terminus prevents the protein from functioning in the vulval epithelia but does not prevent it from functioning to regulate GLR-1 localization in neurons. Finally, we show that human Mint2 can substitute for LIN-10 to facilitate GLR-1 localization in neurons and that the Mint2 amino terminus is critical for this function. Together, our data suggest that LIN-10 uses distinct modular domains for its functions in neurons and epithelial cells and that during evolution its vertebrate ortholog Mint2 has retained the ability to direct AMPAR localization in neurons.
机译:α-氨基-3-羟基-5-甲基-4-异恶唑丙酸(AMPA)型谷氨酸受体(AMPARs)介导神经元突触的兴奋性神经传递,其受调节的定位在突触可塑性中起作用。在秀丽隐杆线虫中,对于AMPAR亚基GLR-1的突触定位和上皮中的外来命运的诱导,都需要包含PDZ和PTB结构域的蛋白LIN-10。在这里,我们研究了不同的LIN-10域在GLR-1本地化中的作用。我们发现,LIN-10的氨基末端区域将LIN-10蛋白定位到高尔基体和突触簇。此外,羧基末端PDZ结构域中的突变可阻止LIN-10调节神经元中的GLR-1定位,但不会阻止LIN-10在外阴上皮细胞中起作用。氨基末端的突变会阻止蛋白质在外阴上皮细胞中起作用,但不会阻止其在神经元中调节GLR-1的位置。最后,我们证明了人类Mint2可以替代LIN-10来促进神经元中的GLR-1定位,并且Mint2氨基末端对于该功能至关重要。总之,我们的数据表明LIN-10在神经元和上皮细胞中的功能使用了独特的模块化结构域,并且在进化过程中其脊椎动物直系同源物Mint2保留了指导AMPAR在神经元中定位的能力。

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