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整合素 α5β1 对于调控小鼠大脑发育过程中皮质神经元的放射状迁移是必需的。

Integrin alpha5beta1 is necessary for regulation of radial migration of cortical neurons during mouse brain development.

机构信息

Institut de Génétique et de Biologie Moléculaire et Cellulaire, Department of Cell Biology and Development, CNRS UMR7104, Inserm U964, Université de Strasbourg, 67404 Illkirch, France.

出版信息

Eur J Neurosci. 2010 Feb;31(3):399-409. doi: 10.1111/j.1460-9568.2009.07072.x. Epub 2010 Jan 25.

Abstract

During cerebral cortex development, post-mitotic neurons interact with radial glial fibers and the extracellular environment to migrate away from the ventricular region and form a correct laminar structure. Integrin receptors are major mediators of cell-cell and cell-extracellular matrix interactions. Several integrin heterodimers are present during formation of the cortical layers. The alpha5beta1 receptor is expressed in the neural progenitors of the ventricular zone during cerebral cortex formation. Using in utero electroporation to introduce short hairpin RNAs in the brain at embryonic day 15.5, we were able to inhibit acutely the expression of alpha5 integrin in the developing cortex. The knockdown of alpha5 integrin expression level in neural precursors resulted in an inhibition of radial migration, without perturbing the glial scaffold. Moreover, the same inhibitory effect on neuronal migration was observed after electroporation of a Cre recombinase expression plasmid into the neural progenitors of conditional knockout mice for alpha5 integrin. In both types of experiments, the electroporated cells expressing reduced levels of alpha5 integrin accumulated in the premigratory region with an abnormal morphology. At postnatal day 2, ectopic neurons were observed in cortical layer V, while a deficit of neurons was observed in cortical layer II-IV. We show that these neurons do not express a layer V-specific marker, suggesting that they have not undergone premature differentiation. Overall, these results indicate that alpha5beta1 integrin functions in the regulation of neural morphology and migration during cortical development, playing a role in cortical lamination.

摘要

在大脑皮层发育过程中,有丝分裂后的神经元与放射状胶质纤维和细胞外环境相互作用,从而从脑室区域迁移出去,并形成正确的层状结构。整合素受体是细胞-细胞和细胞-细胞外基质相互作用的主要介质。在皮质层形成过程中存在几种整合素异二聚体。α5β1 受体在大脑皮层形成过程中表达于脑室区的神经祖细胞中。通过在胚胎第 15.5 天向大脑内进行电穿孔导入短发夹 RNA,我们能够在发育中的皮质中急性抑制 α5 整合素的表达。神经前体细胞中 α5 整合素表达水平的敲低导致放射状迁移受到抑制,而不会干扰神经胶质支架。此外,在条件性敲除 α5 整合素的小鼠的神经前体细胞中电穿孔 Cre 重组酶表达质粒后,也观察到对神经元迁移的相同抑制作用。在这两种实验类型中,表达水平降低的 α5 整合素的电穿孔细胞在迁移前区积聚,形态异常。在出生后第 2 天,观察到皮质 V 层中有异位神经元,而在皮质 II-IV 层中观察到神经元缺失。我们表明这些神经元不表达 V 层特异性标志物,表明它们没有经历过早分化。总的来说,这些结果表明,α5β1 整合素在大脑皮层发育过程中调节神经形态和迁移,在皮层分层中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1d49/3562477/99309311fd06/ejn0031-0399-f1.jpg

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