Engineering GPCR signaling pathways with RASSLs

被引:187
|
作者
Conklin, Bruce R.
Hsiao, Edward C.
Claeysen, Sylvie
Dumuis, Aline
Srinivasan, Supriya
Forsayeth, John R.
Guettier, Jean-Marc
Chang, W. C.
Pei, Ying
McCarthy, Ken D.
Nissenson, Robert A.
Wess, Juergen
Bockaert, Joeal
Roth, Bryan L.
机构
[1] Gladstone Inst Cardiovasc Dis, San Francisco, CA 94158 USA
[2] Univ Calif San Francisco, Dept Med, San Francisco, CA 94122 USA
[3] Univ Calif San Francisco, Dept Cellular, San Francisco, CA 94122 USA
[4] Univ Calif San Francisco, Dept Mol Pharmacol, San Francisco, CA 94122 USA
[5] Univ Calif San Francisco, Vet Affairs Med Ctr, Endocrine Res Unit, San Francisco, CA 94121 USA
[6] Univ Calif San Francisco, Dept Med, San Francisco, CA 94121 USA
[7] Univ Calif San Francisco, Dept Physiol, San Francisco, CA 94121 USA
[8] CNRS, UMR 5203, Inst Genom Fonctionnelle, F-34094 Montpellier, France
[9] Inst Natl Sante & Rech Med, U661, F-34094 Montpellier, France
[10] Univ Montpellier, F-34094 Montpellier, France
[11] Univ Calif San Francisco, Dept Physiol, San Francisco, CA 94143 USA
[12] Univ Calif San Francisco, Dept Neurosurg, San Francisco, CA 94103 USA
[13] NIDDKD, Bioorgan Chem Lab, NIH, Bethesda, MD 20892 USA
[14] Univ Calif San Francisco, Grad Program Pharmaceut Sci & Pharmacogenom, San Francisco, CA 94143 USA
[15] Univ N Carolina, Dept Pharmacol, Chapel Hill, NC 27599 USA
关键词
D O I
10.1038/nmeth.1232
中图分类号
Q5 [生物化学];
学科分类号
071010 ; 081704 ;
摘要
We are creating families of designer G protein coupled receptors (GPCRs) to allow for precise spatiotemporal control of GPCR signaling in vivo. These engineered GPCRs, called receptors activated solely by synthetic ligands (RASSLs), are unresponsive to endogenous ligands but can be activated by nanomolar concentrations of pharmacologically inert, drug-like small molecules. Currently, RASSLs exist for the three major GPCR signaling pathways (G(s), G(i) and G(q)). We review these advances here to facilitate the use of these powerful and diverse tools.
引用
收藏
页码:673 / 678
页数:6
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