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首页> 外文期刊>Journal of receptor and signal transduction research >Cellular models for the study of the pharmacology and signaling of melanin-concentrating hormone receptors
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Cellular models for the study of the pharmacology and signaling of melanin-concentrating hormone receptors

机译:用于研究黑色素浓缩激素受体的药理学和信号传导的细胞模型

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摘要

Cellular models for the study of the neuropeptide melanin-concentrating hormone (MCH) have become indispensable tools for pharmacological profiling and signaling analysis of MCH and its synthetic analogues. Although expression of MCH receptors is most abundant in the brain, MCH-R_1 is also found in different peripheral tissues. Therefore, not only cell lines derived from nervous tissue but also from peripheral tissues that naturally express MCH receptors have been used to study receptor signaling and regulation. For screening of novel compounds, however, heterologous expression of MCH-R _1 or MCH-R_2 genes in HEK293, Chinese hamster ovary, COS-7, or 3T3-L1 cells, or amplified MCH-R_1 expression/signaling in IRM23 cells transfected with the G_q protein gene are the preferred tools because of more distinct pharmacological effects induced by MCH, which include inhibition of cAMP formation, stimulation of inositol triphosphate production, increase in intracellular free Ca~(2+) and/or activation of mitogen-activated protein kinases. Most of the published data originate from this type of model system, whereas data based on studies with cell lines endogenously expressing MCH receptors are more limited. This review presents an update on the different cellular models currently used for the analysis of MCH receptor interaction and signaling.
机译:研究神经肽黑色素浓缩激素(MCH)的细胞模型已成为MCH及其合成类似物的药理分析和信号分析的必不可少的工具。尽管MCH受体的表达在大脑中最为丰富,但在不同的外周组织中也发现了MCH-R_1。因此,不仅使用源自神经组织的细胞系,而且使用天然表达MCH受体的外周组织的细胞系来研究受体的信号传导和调节。但是,为了筛选新型化合物,可在HEK293,中国仓鼠卵巢,COS-7或3T3-L1细胞中异源表达MCH-R _1或MCH-R_2基因,或在经MHC-R_1转染的IRM23细胞中扩增MCH-R_1表达/信号。 G_q蛋白基因是首选的工具,因为MCH可以诱导更明显的药理作用,包括抑制cAMP的形成,刺激三磷酸肌醇的产生,细胞内游离Ca〜(2+)的增加和/或丝裂原活化蛋白的激活激酶。大多数公开的数据都来自这种类型的模型系统,而基于对内源性表达MCH受体的细胞系的研究得到的数据则更为有限。这项审查提出了当前用于MCH受体相互作用和信号分析的不同细胞模型的更新。

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