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特定的β1整合素介导源自胚胎纹状体的神经祖细胞的黏附、迁移和分化。

Specific beta1 integrins mediate adhesion, migration, and differentiation of neural progenitors derived from the embryonic striatum.

作者信息

Tate Matthew C, García Andrés J, Keselowsky Benjamin G, Schumm Michael A, Archer David R, LaPlaca Michelle C

机构信息

Coulter Department of Biomedical Engineering, Georgia Institute of Technology, Atlanta, GA 30332-0535, USA.

出版信息

Mol Cell Neurosci. 2004 Sep;27(1):22-31. doi: 10.1016/j.mcn.2004.05.001.

Abstract

Early inductive signals within the embryonic mammalian forebrain establish two major germinal regions along the dorsal-ventral axis. The dorsal germinal zone eventually forms the cerebral cortex while the ventral ganglionic eminence primarily forms the striatum and globus pallidus. The mechanisms leading to patterning of specific forebrain structures from these distinct germinal regions are not fully understood but may involve the adhesive and migratory properties of regionally specified cells and their interactions with the extracellular environments in which they reside. In the present study, we isolated ganglionic eminence neural progenitor cells (geNPC), precursors of the adult striatum, from the ventral forebrain germinal zone and analyzed adhesion, migration, and differentiation of geNPC on various extracellular matrix (ECM) substrates in vitro. Specifically, we evaluated the role of beta1 integrins, a family of cell surface receptors important in neural development, in mediating geNPC behavior on ECM molecules expressed in embryonic brain tissue. Adhesion and migration of geNPC were significantly enhanced on laminin (LN) and fibronectin (FN) relative to other ECM substrates. Antibody perturbation experiments revealed that although geNPC express several beta1 integrins (alpha1beta1, alpha2beta1, alpha3beta1, alpha5beta1, alpha6beta1, alphavbeta1), adhesion and migration on LN and FN were primarily mediated by alpha6beta1 and alpha5beta1, respectively, and these interactions were confirmed by biochemical cross-link/extraction procedures. Finally, neuronal differentiation of geNPC was enhanced on LN, indicating a role for LN in geNPC differentiation. beta1 integrin-ECM interactions may contribute to basic mechanisms of striatal development and may explain the potent migratory capacity of geNPC transplanted into the adult brain.

摘要

胚胎期哺乳动物前脑内的早期诱导信号沿背腹轴建立了两个主要的生发区。背侧生发区最终形成大脑皮层,而腹侧神经节隆起主要形成纹状体和苍白球。从这些不同的生发区形成特定前脑结构的机制尚未完全了解,但可能涉及区域特异性细胞的黏附与迁移特性以及它们与所处细胞外环境的相互作用。在本研究中,我们从腹侧前脑生发区分离出神经节隆起神经祖细胞(geNPC),即成年纹状体的前体细胞,并在体外分析了geNPC在各种细胞外基质(ECM)底物上的黏附、迁移和分化情况。具体而言,我们评估了β1整合素(在神经发育中起重要作用的一类细胞表面受体)在介导geNPC对胚胎脑组织中表达的ECM分子的行为方面的作用。相对于其他ECM底物,geNPC在层粘连蛋白(LN)和纤连蛋白(FN)上的黏附与迁移显著增强。抗体干扰实验表明,尽管geNPC表达多种β1整合素(α1β1、α2β1、α3β1、α5β1、α6β1、αvβ1),但在LN和FN上的黏附与迁移分别主要由α6β1和α5β1介导,并且这些相互作用通过生化交联/提取程序得到了证实。最后,geNPC在LN上的神经元分化增强,表明LN在geNPC分化中发挥作用。β1整合素与ECM的相互作用可能有助于纹状体发育的基本机制,并可能解释移植到成年大脑中的geNPC的强大迁移能力。

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