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松弛素家族肽的受体。

Receptors for relaxin family peptides.

作者信息

Bathgate Ross A, Ivell Richard, Sanborn Barbara M, Sherwood O David, Summers Roger J

机构信息

Howard Florey Institute of Experimental Physiology and Medicine, University of Melbourne, Victoria 3010, Australia.

出版信息

Ann N Y Acad Sci. 2005 May;1041:61-76. doi: 10.1196/annals.1282.010.

Abstract

Recent studies have identified four receptors that are the physiological targets for relaxin family peptides. All are class I (rhodopsin like) G-protein-coupled receptors with LGR7 (RXFP1) and LGR8 (RXFP2) being type C leucine-rich repeat-containing receptors, whereas GPCR135 (RXFP3) and GPCR142 (RXFP4) resemble receptors that respond to small peptides such as somatostatin and angiotensin II. The cognate ligands for the receptors have been identified: relaxin for RXFP1; INSL3 for RXFP2; relaxin 3 for RXFP3 and INSL5 for RXFP4. RXFP1 and RXFP2 receptors produce increases in intracellular cAMP levels upon stimulation, although the response is complex and contains a component sensitive to PI-3-kinase inhibitors. There is also evidence that RXFP1 can activate Erk1/2 and nitric oxide synthase, and relaxin has been reported to enter cells and activate glucocorticoid receptors. In contrast, RXFP3 and RXFP4 couple to Gi by a pertussis toxin-sensitive mechanism to cause inhibition of cAMP production. Now that the receptors for relaxin family peptides and their cognate ligands have been identified, we suggest a nomenclature for both the peptides and the receptors that we hope will be helpful to researchers in this rapidly advancing field.

摘要

最近的研究已经确定了四种受体,它们是松弛素家族肽的生理靶点。所有这些受体都是I类(视紫红质样)G蛋白偶联受体,其中LGR7(RXFP1)和LGR8(RXFP2)是含C型富亮氨酸重复序列的受体,而GPCR135(RXFP3)和GPCR142(RXFP4)类似于对生长抑素和血管紧张素II等小肽有反应的受体。这些受体的同源配体已被确定:RXFP1的配体是松弛素;RXFP2的配体是胰岛素样肽3(INSL3);RXFP3的配体是松弛素3;RXFP4的配体是胰岛素样肽5(INSL5)。RXFP1和RXFP2受体在受到刺激后会使细胞内cAMP水平升高,尽管这种反应很复杂,并且包含对PI-3激酶抑制剂敏感的成分。也有证据表明RXFP1可以激活细胞外信号调节激酶1/2(Erk1/2)和一氧化氮合酶,并且有报道称松弛素可以进入细胞并激活糖皮质激素受体。相比之下,RXFP3和RXFP4通过一种对百日咳毒素敏感的机制与Gi偶联,从而抑制cAMP的产生。既然已经确定了松弛素家族肽的受体及其同源配体,我们建议为这些肽和受体命名,希望这将对这个快速发展领域的研究人员有所帮助。

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