Hébert Terence E
Department of Pharmacology and Therapeutics, Faculty of Medicine, 13th floor, Room 1303, McIntyre Medical Sciences Building, 3655 Promenade Sir William Osler, Montreal, QC, Canada, H3G 1Y6.
Biochem J. 2008 Jun 1;412(2):e7-9. doi: 10.1042/BJ20080620.
Heterodimerization of GPCRs (G-protein-coupled receptors) has begun to be appreciated as a rich new vein for drug discovery. The possibility of developing modulators for different GPCRs which work at allosteric sites other than the ligand-binding site is not new, but the notion of using a dimeric receptor partner as the target for this intervention has not yet percolated into the broader industrial community. In the present article, I discuss this notion in the context of the heterodimeric delta-opioid receptor-CXCR2 chemokine receptor dimer identified by Parenty et al., in this issue of the Biochemical Journal.
G蛋白偶联受体(GPCRs)的异源二聚化已开始被视为药物发现的一条丰富的新途径。开发作用于配体结合位点以外变构位点的不同GPCR调节剂的可能性并不新鲜,但将二聚体受体伴侣作为这种干预靶点的概念尚未渗透到更广泛的工业界。在本文中,我将结合Parenty等人在本期《生物化学杂志》中鉴定的异源二聚体δ-阿片受体-CXCR2趋化因子受体二聚体来讨论这一概念。
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