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Pannexin 2 由出生后海马神经祖细胞表达,并调节神经元的定型。

Pannexin 2 is expressed by postnatal hippocampal neural progenitors and modulates neuronal commitment.

机构信息

Department of Biochemistry, Neural Regeneration Laboratory and Ottawa Institute of Systems Biology, University of Ottawa, Ottawa, Ontario K1M 1E5, Canada.

出版信息

J Biol Chem. 2010 Aug 6;285(32):24977-86. doi: 10.1074/jbc.M110.130054. Epub 2010 Jun 7.

Abstract

The pannexins (Panx1, -2, and -3) are a mammalian family of putative single membrane channels discovered through homology to invertebrate gap junction-forming proteins, the innexins. Because connexin gap junction proteins are known regulators of neural stem and progenitor cell proliferation, migration, and specification, we asked whether pannexins, specifically Panx2, play a similar role in the postnatal hippocampus. We show that Panx2 protein is differentially expressed by multipotential progenitor cells and mature neurons. Both in vivo and in vitro, Type I and IIa stem-like neural progenitor cells express an S-palmitoylated Panx2 species localizing to Golgi and endoplasmic reticulum membranes. Protein expression is down-regulated during neurogenesis in neuronally committed Type IIb and III progenitor cells and immature neurons. Panx2 is re-expressed by neurons following maturation. Protein expressed by mature neurons is not palmitoylated and localizes to the plasma membrane. To assess the impact of Panx2 on neuronal differentiation, we used short hairpin RNA to suppress Panx2 expression in Neuro2a cells. Knockdown significantly accelerated the rate of neuronal differentiation. Neuritic extension and the expression of antigenic markers of mature neurons occurred earlier in stable lines expressing Panx2 short hairpin RNA than in controls. Together, these findings describe an endogenous post-translational regulation of Panx2, specific to early neural progenitor cells, and demonstrate that this expression plays a role in modulating the timing of their commitment to a neuronal lineage.

摘要

Pannexins(Panx1、-2 和 -3)是一类哺乳动物假定的单通道膜蛋白,通过与无脊椎动物间隙连接形成蛋白——连接蛋白的同源性而被发现。由于连接蛋白间隙连接蛋白是已知的神经干细胞和祖细胞增殖、迁移和特化的调节因子,我们想知道 Pannexin,特别是 Panx2,是否在出生后海马体中发挥类似作用。我们发现 Panx2 蛋白由多能祖细胞和成熟神经元差异表达。在体内和体外,I 型和 IIa 干细胞样神经祖细胞表达一种 S-棕榈酰化 Panx2 物种,定位于高尔基体和内质网膜。在神经元定向的 IIb 和 III 型祖细胞和未成熟神经元中,神经发生过程中蛋白表达下调。成熟神经元重新表达 Panx2。成熟神经元表达的蛋白不发生棕榈酰化,定位于质膜。为了评估 Panx2 对神经元分化的影响,我们使用短发夹 RNA 抑制 Neuro2a 细胞中的 Panx2 表达。敲低显著加速了神经元分化的速度。在表达 Panx2 短发夹 RNA 的稳定系中,神经突延伸和成熟神经元的抗原标记表达比对照更早发生。这些发现共同描述了 Panx2 的一种内源性翻译后调节,特异性地存在于早期神经祖细胞中,并证明这种表达在调节其向神经元谱系分化的时机方面发挥作用。

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