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pcd/pcd小鼠嗅球中细胞迁移和存活的变化。

Changes in cell migration and survival in the olfactory bulb of the pcd/pcd mouse.

作者信息

Valero J, Weruaga E, Murias A R, Recio J S, Curto G G, Gómez C, Alonso J R

机构信息

Lab Plasticidad Neuronal y Neurorreparación, Instituto de Neurociencias de Castilla y León, Universidad de Salamanca, E-37007 Salamanca, Spain.

出版信息

Dev Neurobiol. 2007 Jun;67(7):839-59. doi: 10.1002/dneu.20352.

Abstract

Postnatally, the Purkinje cell degeneration mutant mice lose the main projecting neurons of the main olfactory bulb (OB): mitral cells (MC). In adult animals, progenitor cells from the rostral migratory stream (RMS) differentiate into bulbar interneurons that modulate MC activity. In the present work, we studied changes in proliferation, tangential migration, radial migration patterns, and the survival of these newly generated neurons in this neurodegeneration animal model. The animals were injected with bromodeoxyuridine 2 weeks or 2 months before killing in order to label neuroblast incorporation into the OB and to analyze the survival of these cells after differentiation, respectively. Both the organization and cellular composition of the RMS and the differentiation of the newly generated neurons in the OB were studied using specific markers of glial cells, neuroblasts, and mature neurons. No changes were observed in the cell proliferation rate nor in their tangential migration through the RMS, indicating that migrating neuroblasts are only weakly responsive to the alteration in their target region, the OB. However, the absence of MC does elicit differences in the final destination of the newly generated interneurons. Moreover, the loss of MC also produces changes in the survival of the newly generated interneurons, in accordance with the dramatic decrease in the number of synaptic targets available.

摘要

出生后,浦肯野细胞变性突变小鼠失去了主嗅球(OB)的主要投射神经元:二尖瓣细胞(MC)。在成年动物中,来自吻侧迁移流(RMS)的祖细胞分化为调节MC活性的球内中间神经元。在本研究中,我们研究了这种神经退行性动物模型中这些新生成神经元的增殖、切向迁移、径向迁移模式以及存活情况的变化。在处死前2周或2个月给动物注射溴脱氧尿苷,以便分别标记成神经细胞并入OB的情况,并分析这些细胞分化后的存活情况。使用神经胶质细胞、成神经细胞和成熟神经元的特异性标记物研究了RMS的组织结构和细胞组成以及OB中新生成神经元的分化情况。在细胞增殖率或它们通过RMS的切向迁移方面未观察到变化,这表明迁移的成神经细胞对其靶区域OB的改变反应较弱。然而,MC的缺失确实会引起新生成中间神经元最终目的地的差异。此外,MC的缺失还会导致新生成中间神经元存活情况的变化,这与可用突触靶点数量的急剧减少一致。

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