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首页> 外文期刊>Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation >N-Glycosylation of the Discoidin Domain Receptor Is Required for Axon Regeneration in Caenorhabditis elegans
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N-Glycosylation of the Discoidin Domain Receptor Is Required for Axon Regeneration in Caenorhabditis elegans

机译:在Caenorhabditis elegans的轴突再生需要浮体畴受体的N-糖基化

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摘要

Axon regeneration following neuronal injury is an important repair mechanism that is not well understood at present. In Caenorhabditis elegans, axon regeneration is regulated by DDR-2, a receptor tyrosine kinase (RTK) that contains a discoidin domain and modulates the Met-like SVH-2 RTK-JNK MAP kinase signaling pathway. Here, we describe the svh-10/sqv-3 and svh-11 genes, which encode components of a conserved glycosylation pathway, and show that they modulate axon regeneration in C. elegans. Overexpression of svh-2, but not of ddr-2, can suppress the axon regeneration defect observed in svh-11 mutants, suggesting that SVH-11 functions between DDR-2 and SVH-2 in this glycosylation pathway. Furthermore, we found that DDR-2 is N-glycosylated at the Asn-141 residue located in its discoidin domain, and mutation of this residue caused an axon regeneration defect. These findings indicate that N-linked glycosylation plays an important role in axon regeneration in C. elegans.
机译:神经元损伤后的轴突再生是目前尚未充分理解的重要修复机制。 在皮卡洛伯杆菌中,轴突再生由DDR-2调节,受体酪氨酸激酶(RTK)含有盘状蛋白域,并调节Met样SVH-2 RTK-JNK MAP激酶信号传导途径。 在此,我们描述了SVH-10 / SQV-3和SVH-11基因,其编码保守的糖基化途径的组分,并表明它们在C.杆状此卡中调节轴突再生。 SVH-2的过度表达,但不具有DDR-2,可以抑制在SVH-11突变体中观察到的轴突再生缺陷,表明该糖基化途径中的DDR-2和SVH-2之间的SVH-11功能。 此外,我们发现DDR-2在位于其浮体结构域的ASN-141残基下是N-糖基化,并且该残余物的突变导致轴突再生缺陷。 这些发现表明,N-连接的糖基化在C.杆状此中的轴突再生中起重要作用。

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