G protein-coupled receptors (GPCRs) are flexible integral membrane proteins involved in transmembrane signaling. Their involvement in many physiological processes makes them interesting targets for drug development. Determination of the structure of these receptors will help to design more specific drugs, however, their structural characterization has so far been hampered by the low expression and their inherent instability in detergents which made protein engineering indispensable for structural and biophysical characterization. Several approaches to stabilize the receptors in a particular conformation have led to breakthroughs in GPCR structure determination. These include truncations of the flexible regions, stabilization by antibodies and nanobodies, fusion partners, high affinity and covalently bound ligands as well as conformational stabilization by mutagenesis. In this review we focus on stabilization of GPCRs by insertion of point mutations, which lead to increased conformational and thermal stability as well as improved expression levels. We summarize existing mutagenesis strategies with different coverage of GPCR sequence space and depth of information, design and transferability of mutations and the molecular basis for stabilization. We also discuss whether mutations alter the structure and pharmacological properties of GPCRs.
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Leiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, NetherlandsLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
Bongers, B. J.
Gonzalez, M. Gorostiola
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Leiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
ONCODE Inst, Leiden, NetherlandsLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
Gonzalez, M. Gorostiola
Wang, X.
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Leiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, NetherlandsLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
Wang, X.
van Vlijmen, H. W. T.
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Leiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
Janssen Pharmaceut NV, Beerse, BelgiumLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
van Vlijmen, H. W. T.
Jespers, W.
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Leiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
Uppsala Univ, Dept Cell & Mol Biol, Uppsala, SwedenLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
Jespers, W.
Gutierrez-de-Teran, H.
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Uppsala Univ, Dept Cell & Mol Biol, Uppsala, SwedenLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
Gutierrez-de-Teran, H.
Ye, K.
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Xi An Jiao Tong Univ, Sch Elect & Informat Engn, Xian, Peoples R ChinaLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
Ye, K.
IJzerman, A. P.
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Leiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, NetherlandsLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
IJzerman, A. P.
Heitman, L. H.
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Leiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
ONCODE Inst, Leiden, NetherlandsLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
Heitman, L. H.
van Westen, G. J. P.
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Leiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, NetherlandsLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Leiden, Netherlands
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Beckman Res Inst City Hope, Div Immunol, Duarte, CA 91010 USABeckman Res Inst City Hope, Div Immunol, Duarte, CA 91010 USA
Vaidehi, Nagarajan
Grisshammer, Reinhard
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NINDS, NIH, Dept Hlth & Human Serv, Membrane Prot Struct Funct Unit, Rockville, MD 20852 USABeckman Res Inst City Hope, Div Immunol, Duarte, CA 91010 USA
Grisshammer, Reinhard
Tate, Christopher G.
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Mol Biol Lab, MRC, Cambridge CB2 0QH, EnglandBeckman Res Inst City Hope, Div Immunol, Duarte, CA 91010 USA