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垂体腺苷酸环化酶激活多肽(PACAP)及其在耳蜗中的受体(PAC1-R):大鼠显微解剖耳蜗亚组分中PAC1-R剪接变体特异性转录表达的证据。

Pituitary adenylyl cyclase-activating polypeptide (PACAP) and its receptor (PAC1-R) in the cochlea: evidence for specific transcript expression of PAC1-R splice variants in rat microdissected cochlear subfractions.

作者信息

Abu-Hamdan M D, Drescher M J, Ramakrishnan N A, Khan K M, Toma V S, Hatfield J S, Drescher D G

机构信息

Laboratory of Bio-otology, Department of Otolaryngology, Wayne State University School of Medicine, 261 Lande Medical Research Building, 540 East Canfield Avenue, Detroit, MI 48201, USA.

出版信息

Neuroscience. 2006 Jun 19;140(1):147-61. doi: 10.1016/j.neuroscience.2006.01.019. Epub 2006 Apr 19.

Abstract

Pituitary adenylyl cyclase-activating polypeptide (PACAP) is a neuropeptide originally isolated from the hypothalamus, named for its high potency in stimulating adenylyl cyclase in pituitary cells. PACAP acts through the specific receptor PAC1-R to modulate the action of neurotransmitters, and additionally, to regulate cell viability via autocrine/intracrine mechanisms. Evidence has now been obtained that PACAP and multiple splice variants of PAC1-R are expressed in the rat cochlea. mRNA for PACAP precursor protein is found by reverse transcription-polymerase chain reaction (RT-PCR) in microdissected cochlear lateral wall, organ of Corti, and spiral ganglion subfractions. A specific pattern of expression of mRNA for PAC1-R splice variants, which mediate the response to PACAP, has been revealed by RT-PCR and cloning for the cochlear subfractions. Transcript for the short form of PAC1-R is found in all three subfractions. Four additional splice variants -- hop1, hop2, hip, and a novel hop1 splice variant -- are expressed in the lateral wall. For the amino terminus splice region of PAC1-R, a new splice variant has been detected in the organ of Corti, representing a deletion of the first 7 of 21 amino acids detected in the PAC1-R very-short sequence. Overall, from message determinations in cochlear subfractions, there are five PAC1-R splice variants in the lateral wall, two in the organ of Corti and one in the spiral ganglion, indicating multiple possible responses to PACAP and/or mechanisms to modulate the response to PACAP in the cochlea. The variety of PAC1-R splice variants expressed may reflect the diversity in cell function between subfractions that is modulated by PACAP. The neuropeptide and its specific receptor have been immunolocalized in the lateral wall, the source of the largest number of cochlear PAC1-R splice variants. The receptor was targeted by primary antibodies which would elicit immunoreactivity for all splice variants of PAC1-R detected with RT-PCR, and evidence has been obtained with Western blot analysis suggesting that PAC1-R is glycosylated in vivo. Within the lateral wall, PACAP and PAC1-R were immunolocalized primarily to the stria vascularis, with immunoreactivity for both neuropeptide and receptor increasing from the basal to apical cochlear turns. Within the stria, PACAP immunoreactivity was localized to the basolateral extensions of marginal cells, while PAC1-R was clearly associated with tight junctions between the marginal cells close to the endolymphatic compartment. In addition, evidence was obtained that PAC1-R was associated with endothelial cells of the capillaries in the stria vascularis. The large number of splice variants expressed, coupled to the specificity in linkage between PAC1-R splice variants and G-protein-coupled second messenger pathways, could provide a mechanism to closely modulate tight junction integrity in the stria vascularis, impacting the endolymphatic potential.

摘要

垂体腺苷酸环化酶激活多肽(PACAP)是一种最初从下丘脑分离出的神经肽,因其在刺激垂体细胞中的腺苷酸环化酶方面具有高效能而得名。PACAP通过特异性受体PAC1-R发挥作用,调节神经递质的作用,此外,还通过自分泌/内分泌机制调节细胞活力。现已获得证据表明,PACAP和PAC1-R的多种剪接变体在大鼠耳蜗中表达。通过逆转录聚合酶链反应(RT-PCR)在显微解剖的耳蜗外侧壁、柯蒂氏器和螺旋神经节亚组分中发现了PACAP前体蛋白的mRNA。RT-PCR和克隆已揭示了介导对PACAP反应的PAC1-R剪接变体在耳蜗亚组分中的特定表达模式。在所有三个亚组分中均发现了PAC1-R短形式的转录本。另外四种剪接变体——hop1、hop2、hip和一种新的hop1剪接变体——在外侧壁中表达。对于PAC1-R的氨基末端剪接区域,在柯蒂氏器中检测到一种新的剪接变体,它代表在PAC1-R极短序列中检测到的21个氨基酸中的前7个氨基酸的缺失。总体而言,从耳蜗亚组分中的信息测定来看,外侧壁中有五种PAC1-R剪接变体,柯蒂氏器中有两种,螺旋神经节中有一种,这表明在耳蜗中对PACAP有多种可能的反应和/或调节对PACAP反应的机制。所表达的PAC1-R剪接变体的多样性可能反映了由PACAP调节的亚组分之间细胞功能的差异。该神经肽及其特异性受体已在外侧壁中进行了免疫定位,外侧壁是耳蜗中PAC1-R剪接变体数量最多的来源。该受体由能引发对通过RT-PCR检测到的PAC1-R所有剪接变体免疫反应性的一抗靶向,并且蛋白质印迹分析已获得证据表明PAC1-R在体内被糖基化。在外侧壁内,PACAP和PAC1-R主要定位于血管纹,神经肽和受体的免疫反应性从耳蜗基部到顶部逐渐增加。在血管纹内,PACAP免疫反应性定位于边缘细胞的基底外侧延伸部分,而PAC1-R明显与靠近内淋巴腔的边缘细胞之间的紧密连接相关。此外,已获得证据表明PAC1-R与血管纹中毛细血管的内皮细胞相关。所表达的大量剪接变体,加上PAC1-R剪接变体与G蛋白偶联的第二信使途径之间连接的特异性,可能提供一种机制来紧密调节血管纹中的紧密连接完整性,从而影响内淋巴电位。

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