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交感神经元中垂体腺苷酸环化酶激活多肽(PACAP)调控的基因靶点的微阵列分析。

Microarray analyses of pituitary adenylate cyclase activating polypeptide (PACAP)-regulated gene targets in sympathetic neurons.

作者信息

Braas Karen M, Schutz Kristin C, Bond Jeffrey P, Vizzard Margaret A, Girard Beatrice M, May Victor

机构信息

Department of Anatomy and Neurobiology, The University of Vermont College of Medicine, Burlington, VT 05405, United States.

出版信息

Peptides. 2007 Sep;28(9):1856-70. doi: 10.1016/j.peptides.2007.04.004. Epub 2007 Apr 19.

Abstract

The high and preferential expression of the PAC(1)(short)HOP1 receptor in postganglionic sympathetic neurons facilitates microarray studies for mechanisms underlying PACAP-mediate neurotrophic signaling in a physiological context. Replicate primary sympathetic neuronal cultures were treated with 100 nM PACAP27 either acutely (9 h) or chronically (96 h) before RNA extraction and preparation for Affymetrix microarray analysis. Compared to untreated control cultures, acute PACAP treatment modulated significantly the expression of 147 transcripts of diverse functional groups, including peptides, growth factors/cytokines, transcriptional factors, receptors/signaling effectors and cell cycle regulators, that collectively appeared to facilitate neuronal plasticity, differentiation and/or regeneration processes. Some regulated transcripts, for example, were related to BDNF/TrkB, IL-6/Jak2/Socs2 and TGF/follistatin signaling; many transcripts affected bioactive peptide and polyamine biosynthesis. Although chronic PACAP treatments altered the expression of 109 sympathetic transcripts, only 43 transcripts were shared between the acute and chronic treatment data sets. The PACAP-mediated changes in transcript expression were corroborated independently by quantitative PCR measurement. The PACAP-regulated transcripts in sympathetic neurons did not bear strong resemblance to those in PACAP-treated pheochromocytoma cells. However, many PACAP-targeted sympathetic transcripts, especially those related to peptide plasticity and nerve regeneration processes, coincided significantly with genes altered after peripheral nerve injury. The ability for sympathetic PAC(1)(short)HOP1 receptors to engage multiple downstream signaling cascades appeared to be reflected in the number and diversity of genes targeted in a multifaceted strategy for comprehensive neurotrophic responses.

摘要

节后交感神经元中PAC(1)(short)HOP1受体的高表达及优先表达,有助于在生理背景下对PACAP介导的神经营养信号传导机制进行微阵列研究。在提取RNA并准备用于Affymetrix微阵列分析之前,将复制的原代交感神经元培养物分别急性(9小时)或慢性(96小时)用100 nM PACAP27处理。与未处理的对照培养物相比,急性PACAP处理显著调节了147种不同功能组转录本的表达,这些功能组包括肽、生长因子/细胞因子、转录因子、受体/信号效应器和细胞周期调节因子,它们共同似乎有助于神经元可塑性、分化和/或再生过程。例如,一些受调节的转录本与BDNF/TrkB、IL-6/Jak2/Socs2和TGF/卵泡抑素信号传导有关;许多转录本影响生物活性肽和多胺的生物合成。虽然慢性PACAP处理改变了109种交感神经转录本的表达,但急性和慢性处理数据集之间仅共有43种转录本。通过定量PCR测量独立证实了PACAP介导的转录本表达变化。交感神经元中PACAP调节的转录本与PACAP处理的嗜铬细胞瘤细胞中的转录本没有很强的相似性。然而,许多PACAP靶向的交感神经转录本,尤其是那些与肽可塑性和神经再生过程相关的转录本,与周围神经损伤后改变的基因显著重合。交感神经PAC(1)(short)HOP1受体参与多个下游信号级联反应的能力,似乎反映在针对全面神经营养反应的多方面策略中所靶向的基因数量和多样性上。

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