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神经视网膜中表达 PAC1 的结构在出生后发育过程中改变其 PAC1 同工型的剪接。

PAC1-expressing structures of neural retina alter their PAC1 isoform splicing during postnatal development.

机构信息

Department of Experimental Zoology and Neurobiology, University of Pécs, 6 Ifjúság Street, 7601, Pécs, Hungary,

出版信息

Cell Tissue Res. 2014 Feb;355(2):279-88. doi: 10.1007/s00441-013-1761-0. Epub 2013 Dec 20.

DOI:10.1007/s00441-013-1761-0
PMID:24352804
Abstract

Pituitary adenylate cyclase-activating polypeptide (PACAP), a member of the secretin/glucagon/vasoactive intestinal peptide family, exerts various effects on neuronal development as mediated by the differential expression of PAC1 receptor (PAC1-R) isoforms. The expression changes of PAC1-R isoforms (Hip, Hop1) reported in correlation with retinal development suggest an isoform switch during the second postnatal week. Our aim is to determine the exact period of the isoform shift and to describe the PAC1-R-immunoreactive structures appearing from postnatal day 5 (P5) to P10 in the rat retina. The ratio of Hip and Hop1 receptors was assessed and changes in their expression were followed by Taqman and SybrGreen-based quantitative polymerase chain reaction. For the detection of PAC1-R-expressing retinal structures, anti-PAC1-R, anti-calbindin, anti-protein kinase C, anti-glutamine synthetase, anti-HPC1 and anti-Brn3a antibodies were utilized. At the transcript level, a marked decrease to an undetectable level was measured in Hip mRNA expression from P6 to P9. Hop1 expression appeared to be unchanged from P6 to P9, followed by a significant elevation at P10. A Hip/Hop1 isoform shift occurred between P6 and P7. Immunostaining showed strong PAC1-R labeling from P5 to P10 in ganglion, amacrine, horizontal and rod bipolar neurons and in glial Muller cell processes. The Hop1 isoform was predominantly expressed in various types of retinal cell beginning at P7, because of a dramatic reduction in Hip mRNA level. As the Hop1 receptor is coupled to different signaling cascades, this isoform shift might alter the physiological role of PACAP during this particular period.

摘要

垂体腺苷酸环化酶激活肽(PACAP)是分泌素/胰高血糖素/血管活性肠肽家族的成员,通过差异表达 PAC1 受体(PAC1-R)异构体发挥各种对神经元发育的作用。与视网膜发育相关的 PAC1-R 异构体(Hip、Hop1)的表达变化表明在第二产后周发生了异构体转换。我们的目的是确定该异构体转换的确切时期,并描述在大鼠视网膜中从出生后第 5 天(P5)到第 10 天出现的 PAC1-R 免疫反应性结构。评估 Hip 和 Hop1 受体的比例,并通过 Taqman 和 SybrGreen 基于定量聚合酶链反应(PCR)来跟踪它们的表达变化。为了检测表达 PAC1-R 的视网膜结构,使用了抗-PAC1-R、抗钙结合蛋白、抗蛋白激酶 C、抗谷氨酰胺合成酶、抗 HPC1 和抗 Brn3a 抗体。在转录水平上,从 P6 到 P9,Hip mRNA 表达明显下降至无法检测的水平。Hop1 表达似乎从 P6 到 P9 没有变化,然后在 P10 时显著升高。Hip/Hop1 异构体转换发生在 P6 和 P7 之间。免疫染色显示,从 P5 到 P10,在神经节细胞、无长突细胞、水平细胞和杆状双极细胞以及胶质 Muller 细胞过程中存在强烈的 PAC1-R 标记。从 P7 开始,Hop1 异构体主要在各种类型的视网膜细胞中表达,因为 Hip mRNA 水平急剧下降。由于 Hop1 受体与不同的信号级联偶联,这种异构体转换可能会改变 PACAP 在这一特定时期的生理作用。

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