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垂体腺苷酸环化酶激活多肽与PAC1受体信号传导可增加中枢和外周神经元中Homer 1a的表达。

Pituitary adenylate cyclase activating polypeptide and PAC1 receptor signaling increase Homer 1a expression in central and peripheral neurons.

作者信息

Girard Beatrice M, Keller Emily T, Schutz Kristin C, May Victor, Braas Karen M

机构信息

Departments of Anatomy and Neurobiology, and Pharmacology, University of Vermont College of Medicine, 149 Beaumont Avenue, HSRF 428, Burlington, VT 05405, USA.

出版信息

Regul Pept. 2004 Dec 15;123(1-3):107-16. doi: 10.1016/j.regpep.2004.05.024.

Abstract

Pituitary adenylate cyclase activating polypeptides (PACAP) and PAC1 receptor signaling have diverse roles in central and peripheral nervous system development and function. In recent microarray analyses for PACAP and PAC1 receptor modulation of neuronal transcripts, the mRNA of Homer 1a (H1a), which encodes the noncrosslinking and immediate early gene product isoform of Homer, was identified to be strongly upregulated in superior cervical ganglion (SCG) sympathetic neurons. Given the prominent roles of Homer in synaptogenesis, synaptic protein complex assembly and receptor/channel signaling, we have examined the ability for PACAP to induce H1a expression in sympathetic, cortical and hippocampal neurons to evaluate more comprehensively the roles of PACAP in synaptic function. In both central and peripheral neuronal cultures, PACAP peptides increased transiently H1a transcript levels approximately 3.5- to 6-fold. From real-time quantitative PCR measurements, the temporal patterns of PACAP-mediated H1a mRNA induction among the different neuronal cultures appeared similar although the onset of sympathetic H1a transcript expression appeared protracted. The increase in H1a transcripts was accompanied by increases in H1a protein levels. Comparative studies with VIP and PACAP(6-38) antagonist demonstrated that the PACAP effects reflected PAC1 receptor activation and signaling. The PAC1 receptor isoforms expressed in central and peripheral neurons can engage diverse intracellular second messenger systems, and studies using selective signaling pathway inhibitors demonstrated that the cyclic AMP/PKA and MEK/ERK cascades are principal mediators of the PACAP-mediated H1a induction response. In modulating H1a transcript and protein expression, these studies may implicate broad roles for PACAP and PAC1 receptor signaling in synaptic development and plasticity.

摘要

垂体腺苷酸环化酶激活多肽(PACAP)和PAC1受体信号传导在中枢和外周神经系统的发育及功能中具有多种作用。在最近针对PACAP和PAC1受体对神经元转录本调节作用的微阵列分析中,编码荷马蛋白非交联和早期即刻基因产物亚型的荷马1a(H1a)的mRNA,被发现在颈上神经节(SCG)交感神经元中强烈上调。鉴于荷马蛋白在突触形成、突触蛋白复合体组装以及受体/通道信号传导中发挥的重要作用,我们研究了PACAP在交感神经元、皮层神经元和海马神经元中诱导H1a表达的能力,以更全面地评估PACAP在突触功能中的作用。在中枢和外周神经元培养物中,PACAP肽均使H1a转录水平短暂升高约3.5至6倍。通过实时定量PCR测量,尽管交感神经元中H1a转录本表达的起始似乎较为持久,但不同神经元培养物中PACAP介导的H1a mRNA诱导的时间模式看起来相似。H1a转录本的增加伴随着H1a蛋白水平的升高。与血管活性肠肽(VIP)和PACAP(6 - 38)拮抗剂的比较研究表明,PACAP的作用反映了PAC1受体的激活和信号传导。在中枢和外周神经元中表达的PAC1受体亚型可参与多种细胞内第二信使系统,使用选择性信号通路抑制剂的研究表明,环磷酸腺苷/蛋白激酶A(cAMP/PKA)和丝裂原活化蛋白激酶/细胞外信号调节激酶(MEK/ERK)级联反应是PACAP介导的H1a诱导反应的主要介质。在调节H1a转录本和蛋白表达方面,这些研究可能暗示PACAP和PAC1受体信号传导在突触发育和可塑性中具有广泛作用。

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