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首页> 外文期刊>Results and problems in cell differentiation >Orphan receptors and the concept of reverse physiology: discovery of the novel neuropeptide orphanin FQociceptin.
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Orphan receptors and the concept of reverse physiology: discovery of the novel neuropeptide orphanin FQociceptin.

机译:孤儿受体和逆生理的概念:新型神经肽孤儿蛋白FQ / nociceptin的发现。

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摘要

The cloning of numerous orphan members from the supergene family of G protein-coupled receptors implies the existence of many as yet undiscovered neurotransmitters and neuropeptides. Recently, new technologies were developed to isolate natural ligands for orphan receptors, using the receptor as a biological sensor during the purification process. This manuscript will present the concept and technology of an approach which starts from a cloned receptor to ultimately describe the physiological functions of the transmitter system. This strategy inverts the classical order of biomedical research and was thus termed "reverse physiology". The first natural ligand isolated by this strategy is a peptide with significant similarity to the opioid peptides and has been named orphanin FQ or nociceptin (OFQ/NOC). Evidence for characterizing OFQ/NOC as a genuine neuropeptide will be reviewed. OFQ/NOC is biosynthetically derived from a larger precursor protein which may encode additional bioactive peptides. Since its discovery, a large number of studies have described numerous physiological functions of OFQ/NOC. Because of its relation to the opioid system, much attention has been focused on the involvement of OFQ/NOC in nociception, sometimes with controversial results. However, the pharmacological profile of the OFQ/NOC system suggests a clear separation from the opioids. The discovery of OFQ/NOC and the subsequent analyses of its physiological functions is an example which has already been followed by the identification of two other novel neuropeptides. The orphan receptor strategy holds a lot of promises for the postgenomic era, helping to fill the vast amount of sequence data with life.
机译:来自G蛋白偶联受体超基因家族的众多孤儿成员的克隆意味着存在许多尚未发现的神经递质和神经肽。最近,开发了新技术来分离孤儿受体的天然配体,在纯化过程中使用该受体作为生物传感器。该手稿将介绍一种方法的概念和技术,该方法从克隆的受体开始,最终描述发射器系统的生理功能。这种策略颠覆了生物医学研究的经典顺序,因此被称为“逆向生理学”。通过这种策略分离的第一个天然配体是与阿片样肽具有显着相似性的肽,并被命名为孤儿蛋白FQ或伤害感受蛋白(OFQ / NOC)。将审查表征OFQ / NOC为真正的神经肽的证据。 OFQ / NOC是从较大的前体蛋白合成而来的,前体蛋白可能编码其他生物活性肽。自发现以来,大量研究描述了OFQ / NOC的多种生理功能。由于其与阿片样物质系统的关系,人们将很多注意力集中在OFQ / NOC参与伤害感受中,有时还会引起争议的结果。但是,OFQ / NOC系统的药理学特征表明与阿片类物质有明显的分离。 OFQ / NOC的发现及其随后的生理功能分析是一个例子,随后已经鉴定出另外两种新型神经肽。孤儿受体策略在后基因组时代具有许多前景,有助于填补生命中的大量序列数据。

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