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中枢和外周神经突生长在对肝素结合序列与整合素结合序列的偏好上存在差异。

Central and peripheral neurite outgrowth differs in preference for heparin-binding versus integrin-binding sequences.

作者信息

Haugen P K, McCarthy J B, Roche K F, Furcht L T, Letourneau P C

机构信息

Department of Cell Biology, University of Minnesota, Minneapolis 55455.

出版信息

J Neurosci. 1992 Jun;12(6):2034-42. doi: 10.1523/JNEUROSCI.12-06-02034.1992.

DOI:10.1523/JNEUROSCI.12-06-02034.1992
PMID:1607927
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6575928/
Abstract

Neurons of the CNS and PNS differ in their response to fibronectin (FN) and proteolytic fragments of FN. The 33 kDa C-terminal cell and heparin-binding fragment of FN, in particular, is a strong promoter of CNS neurite outgrowth. To define further the neurite-promoting activity of the 33 kDa fragment, and to investigate further the differences between PNS and CNS responses to FN and the 33 kDa fragment, we contrasted neurite outgrowth by CNS and PNS neurons on three synthetic peptides representing sequences from this fragment of FN: two heparin-binding peptides, FN-C/H I and FN-C/H II (McCarthy et al., 1990), and an integrin-binding peptide, CS1 (Humphries et al., 1987). Spinal cord (SC) neurons, from the CNS, differed from dorsal root ganglion (DRG) neurons, from the PNS, with respect to substratum preference for heparin-binding versus integrin-binding peptides. SC neurite outgrowth was greatest on the heparin-binding peptide FN-C/H II, while DRG neurite outgrowth was greatest on the a4 beta 1 integrin-binding peptide CS1. To test whether the difference in substratum preference was due to differences in the molecular mechanism by which SC and DRG neurons interact with the 33 kDa fragment of FN, anti-beta 1 integrin antibodies and/or soluble heparin were added to the cultures as potential inhibitors of integrin-mediated or proteoglycan-mediated interactions with FN. SC neurite outgrowth was much more sensitive to the effect of heparin than anti-beta 1 integrin, indicating SC neurite outgrowth may involve predominantly a heparin-sensitive mechanism.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

中枢神经系统(CNS)和外周神经系统(PNS)的神经元对纤连蛋白(FN)及其蛋白水解片段的反应有所不同。特别是,FN的33 kDa C末端细胞和肝素结合片段是中枢神经系统神经突生长的强力促进剂。为了进一步确定33 kDa片段的神经突促进活性,并进一步研究外周神经系统和中枢神经系统对FN及33 kDa片段反应的差异,我们对比了中枢神经系统和外周神经系统神经元在代表FN该片段序列的三种合成肽上的神经突生长情况:两种肝素结合肽,FN-C/H I和FN-C/H II(麦卡锡等人,1990年),以及一种整合素结合肽,CS1(汉弗莱斯等人,1987年)。来自中枢神经系统的脊髓(SC)神经元与来自外周神经系统的背根神经节(DRG)神经元在对肝素结合肽与整合素结合肽的底物偏好方面存在差异。SC神经突在肝素结合肽FN-C/H II上的生长最为显著,而DRG神经突在α4β1整合素结合肽CS1上的生长最为显著。为了测试底物偏好的差异是否是由于SC和DRG神经元与FN的33 kDa片段相互作用的分子机制不同所致,将抗β1整合素抗体和/或可溶性肝素作为整合素介导或蛋白聚糖介导的与FN相互作用的潜在抑制剂添加到培养物中。SC神经突生长对肝素的作用比抗β1整合素更敏感,表明SC神经突生长可能主要涉及一种对肝素敏感的机制。(摘要截断于250字)

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