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新生大鼠脑的塌陷反应介导蛋白与硫酸软骨素相互作用。

Collapsin response mediator proteins of neonatal rat brain interact with chondroitin sulfate.

作者信息

Franken Sebastian, Junghans Ulrich, Rosslenbroich Volker, Baader Stephan L, Hoffmann Ralf, Gieselmann Volkmar, Viebahn Christoph, Kappler Joachim

机构信息

Rheinische Friedrich-Wilhelms-Universität Bonn, Institut für Physiologische Chemie, Nussallee 11, D-53115 Bonn, Germany.

出版信息

J Biol Chem. 2003 Jan 31;278(5):3241-50. doi: 10.1074/jbc.M210181200. Epub 2002 Nov 19.

DOI:10.1074/jbc.M210181200
PMID:12444086
Abstract

Chondroitin sulfate proteoglycans are structurally and functionally important components of the extracellular matrix of the central nervous system. Their expression in the developing mammalian brain is precisely regulated, and cell culture experiments implicate these proteoglycans in the control of cell adhesion, neuron migration, neurite formation, neuronal polarization, and neuron survival. Here, we report that a monoclonal antibody against chondroitin sulfate-binding proteins from neonatal rat brain recognizes collapsin response mediator protein-4 (CRMP-4), which belongs to a family of proteins involved in collapsin/semaphorin 3A signaling. Soluble CRMPs from neonatal rat brain bound to chondroitin sulfate affinity columns, and CRMP-specific antisera co-precipitated chondroitin sulfate. Moreover, chondroitin sulfate and CRMP-4 were found to be localized immuno-histochemically in overlapping distributions in the marginal zone and the subplate of the cerebral cortex. CRMPs are released to culture supernatants of NTera-2 precursor cells and of neocortical neurons after cell death, and CRMP-4 is strongly expressed in the upper cortical plate of neonatal rat where cell death is abundant. Therefore, naturally occurring cell death is a plausible mechanism that targets CRMPs to the extracellular matrix at certain stages of development. In summary, our data indicate that CRMPs, in addition to their role as cytosolic signal transduction molecules, may subserve as yet unknown functions in the developing brain as ligands of the extracellular matrix.

摘要

硫酸软骨素蛋白聚糖是中枢神经系统细胞外基质在结构和功能上的重要组成部分。它们在发育中的哺乳动物大脑中的表达受到精确调控,细胞培养实验表明这些蛋白聚糖参与细胞黏附、神经元迁移、神经突形成、神经元极化和神经元存活的控制。在此,我们报告一种针对新生大鼠脑硫酸软骨素结合蛋白的单克隆抗体可识别塌陷反应介导蛋白-4(CRMP-4),它属于参与塌陷蛋白/信号素3A信号传导的蛋白家族。新生大鼠脑的可溶性CRMPs与硫酸软骨素亲和柱结合,且CRMP特异性抗血清可共沉淀硫酸软骨素。此外,通过免疫组织化学发现硫酸软骨素和CRMP-4在大脑皮质边缘区和板下区呈重叠分布。细胞死亡后,CRMPs会释放到NTera-2前体细胞和新皮质神经元的培养上清液中,且CRMP-4在新生大鼠细胞死亡丰富的皮质上层板中强烈表达。因此,自然发生的细胞死亡是一种在发育特定阶段将CRMPs靶向细胞外基质的合理机制。总之,我们的数据表明,CRMPs除了作为胞质信号转导分子发挥作用外,在发育中的大脑中作为细胞外基质的配体可能还具有尚未明确的功能。

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Deletion of collapsin response mediator protein 4 results in abnormal layer thickness and elongation of mitral cell apical dendrites in the neonatal olfactory bulb.
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