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神经生长锥的迁移以空间限定且依赖底物的方式需要抗去污剂膜。

Migration of nerve growth cones requires detergent-resistant membranes in a spatially defined and substrate-dependent manner.

作者信息

Nakai Yoko, Kamiguchi Hiroyuki

机构信息

Developmental Brain Science Group, RIKEN Brain Science Institute (BSI), Wako, Saitama, 351-0198, Japan.

出版信息

J Cell Biol. 2002 Dec 23;159(6):1097-108. doi: 10.1083/jcb.200209077.

Abstract

Motility of nerve growth cones (GCs) is regulated by region-specific activities of cell adhesion molecules (CAMs). CAM activities could be modified by their localization to detergent-resistant membranes (DRMs), specialized microdomains enriched in signaling molecules. This paper deals with a question of whether DRMs are involved in GC migration stimulated by three CAMs; L1, N-cadherin (Ncad), and beta1 integrin. We demonstrate that L1 and Ncad are present in DRMs, whereas beta1 integrin is exclusively detected in non-DRMs of neurons and that localization of L1 and Ncad to DRMs is developmentally regulated. GC migration mediated by L1 and Ncad but not by beta1 integrin is inhibited after DRM disruption by micro-scale chromophore-assisted laser inactivation (micro-CALI) of GM1 gangliosides or by pharmacological treatments that deplete cellular cholesterol or sphingolipids, essential components for DRMs. Characteristic morphology of GCs induced by L1 and Ncad is also affected by micro-CALI-mediated DRM disruption. Micro-CALI within the peripheral domain of GCs, or even within smaller areas such as the filopodia and the lamellipodia, is sufficient to impair their migration. However, micro-CALI within the central domain does not affect GC migration. These results demonstrate the region-specific involvement of DRMs in CAM-dependent GC behavior.

摘要

神经生长锥(GCs)的运动性受细胞粘附分子(CAMs)区域特异性活性的调节。CAMs的活性可因其定位于抗去污剂膜(DRMs)而改变,DRMs是富含信号分子的特殊微结构域。本文探讨了DRMs是否参与由三种CAMs(L1、N-钙粘蛋白(Ncad)和β1整合素)刺激的GC迁移问题。我们证明L1和Ncad存在于DRMs中,而β1整合素仅在神经元的非DRMs中检测到,并且L1和Ncad在DRMs中的定位受发育调控。通过GM1神经节苷脂的微尺度发色团辅助激光失活(micro-CALI)或通过消耗细胞胆固醇或鞘脂(DRMs的必需成分)的药物处理破坏DRM后,由L1和Ncad介导的GC迁移受到抑制,而由β1整合素介导的GC迁移不受影响。由L1和Ncad诱导的GC的特征形态也受到micro-CALI介导的DRM破坏的影响。在GC的外周区域内,甚至在诸如丝状伪足和片状伪足等较小区域内进行micro-CALI,足以损害它们的迁移。然而,在中央区域内进行micro-CALI并不影响GC迁移。这些结果证明了DRMs在CAM依赖的GC行为中具有区域特异性作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b47a/2173975/73ae121899a4/200209077f1.jpg

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