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配体诱导的生长锥塌陷:变异型GAP-43肽的放大作用和阻断作用

Ligand-induced growth cone collapse: amplification and blockade by variant GAP-43 peptides.

作者信息

Igarashi M, Li W W, Sudo Y, Fishman M C

机构信息

Developmental Biology Laboratory, Massachusetts General Hospital, Charlestown 02129, USA.

出版信息

J Neurosci. 1995 Aug;15(8):5660-7. doi: 10.1523/JNEUROSCI.15-08-05660.1995.

DOI:10.1523/JNEUROSCI.15-08-05660.1995
PMID:7643208
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6577624/
Abstract

Growth cones are powerful amplifiers for signals from the microenvironment. Their collapse can be triggered by cell surface components of myelin and brain membranes, as well as by soluble ligands, including neurotransmitters. GAP-43 is a protein concentrated on the inner surface of the growth cone membrane. Assayed in isolation, it interacts with the heterotrimeric protein, G(o), and in oocytes it amplifies the effects of ligand-triggered G protein activation. We wished to examine whether GAP-43 serves to amplify signals at the growth cone. The G(o) stimulating region of GAP-43 is encoded in the 10 amino acids (MLCCMRRT-KQ) of the first exon. We examined the effect of this peptide upon chick dorsal root ganglion growth cone collapse and neurite retraction triggered by brain membranes or myelin, as well as by serotonin. We find that application of the GAP-43 1-10 peptide amplifies the effects of all three ligands. The amplification is greater when GAP-43 1-10 is injected intracellularly. Peptides with amino acid substitutions for the two cysteine residues manifest parallel changes in growth cone collapse and G(o) stimulation. In particular, tyrosine or methionine substitutions cause the peptide to inhibit G(o) and to block induced growth cone collapse. The GAP-43 peptides therefore regulate the sensitivity of growth cones to extrinsic signals. The modified peptides serve as a starting point for the design of reagents to enhance CNS regeneration.

摘要

生长锥是微环境信号的强大放大器。它们的塌陷可由髓磷脂和脑膜的细胞表面成分以及可溶性配体(包括神经递质)触发。GAP - 43是一种集中在生长锥膜内表面的蛋白质。单独检测时,它与异源三聚体蛋白G(o)相互作用,并且在卵母细胞中它会放大配体触发的G蛋白激活的效应。我们希望研究GAP - 43是否在生长锥处放大信号。GAP - 43的G(o)刺激区域由第一个外显子的10个氨基酸(MLCCMRRT - KQ)编码。我们研究了该肽对由脑膜、髓磷脂以及血清素触发的鸡背根神经节生长锥塌陷和神经突回缩的影响。我们发现应用GAP - 43 1 - 10肽会放大所有三种配体的效应。当GAP - 43 1 - 10肽被细胞内注射时,放大作用更强。对两个半胱氨酸残基进行氨基酸替换的肽在生长锥塌陷和G(o)刺激方面表现出平行变化。特别是,酪氨酸或甲硫氨酸替换会使该肽抑制G(o)并阻止诱导的生长锥塌陷。因此,GAP - 43肽调节生长锥对外源信号的敏感性。这些修饰后的肽可作为设计增强中枢神经系统再生试剂的起点。