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Transcriptome of pituitary adenylate cyclase-activating polypeptide-differentiated PC12 cells.

机译:垂体腺苷酸环化酶激活多肽分化的PC12细胞的转录组。

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Addition of pituitary adenylate cyclase-activating polypeptide (PACAP) into the cultured PC12 cells secreted dopamine and promoted neurite outgrowth of the cells, indicating cell differentiation. To characterize the PACAP-differentiated PC12 cell transcriptome, we applied DNA macroarray techniques, using Atlas Rat 1.2 Array membranes (BD Biosciences Clontech) that have 1176 cDNA. RNA samples were harvested from PC12 cells before and at a time of 6 h treatment with 1 nM PACAP, when neuritogenesis was remarkably observed under the condition used. Several genes regulated by PACAP have been associated with neuritogenesis (i.e. villin 2 and tissue plasminogen activator) or cell growth/differentiation (i.e. cyclin or ornitine decarboxylase). Also, cytoskeleton proteins such as actin or tubulin were up-regulated for cell morphology remodeling. A message of vehicle trafficking molecule (synaptotagmin IV) was more remarkably increased (3.95-6.85-fold). Signaling molecules such as small G proteins (rab12, rab16,or ral), IkappaB, or STAT3 were altered by PACAP. It is noteworthy that PACAP inhibited the expression of galanin receptor 2, whose ligand was shown to inhibit tyrosine hydroxylase activity. Thus, in this study the transcriptome of PACAP-differentiated PC12 was established, leading to the elucidation of the molecular mechanism of neuritogenesis by the neuropeptide.
机译:将垂体腺苷酸环化酶激活多肽(PACAP)添加到培养的PC12细胞中会分泌多巴胺并促进神经突向外生长,表明细胞分化。为了表征PACAP分化的PC12细胞转录组,我们使用了具有1176个cDNA的Atlas Rat 1.2阵列膜(BD Biosciences Clontech)应用了DNA宏阵列技术。当在所用条件下显着观察到神经发生时,在用1 nM PACAP处理6h之前和6h时,从PC12细胞中收获RNA样品。由PACAP调节的几种基因与神经形成(即villin 2和组织纤溶酶原激活物)或细胞生长/分化(即细胞周期蛋白或鸟氨酸脱羧酶)有关。同样,细胞骨架蛋白如肌动蛋白或微管蛋白也被上调以进行细胞形态重塑。媒介物运输分子(突触素IV)的信息显着增加(3.95-6.85倍)。信号分子,例如小G蛋白(rab12,rab16或ral),IkappaB或STAT3被PACAP改变。值得注意的是,PACAP抑制了甘丙肽受体2的表达,甘丙肽受体2的配体显示出抑制酪氨酸羟化酶活性的作用。因此,在本研究中,建立了PACAP分化的PC12的转录组,从而阐明了神经肽对神经形成的分子机制的影响。

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