G proteins as drug targets

被引:0
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作者
C. Höller
M. Freissmuth
C. Nanoff
机构
[1] University of Vienna,Institute of Pharmacology
关键词
Key words. G protein subunits; modified guanine nucleotides; receptor-derived peptides; mastoparan and related venoms; suramin analogues; amphiphilic cations.;
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摘要
The structure and function of heterotrimeric G protein subunits is known in considerable detail. Upon stimulation of a heptahelical receptor by the appropriate agonists, the cognate G proteins undergo a cycle of activation and deactivation; the α-subunits and the βγ-dimers interact sequentially with several reaction partners (receptor, guanine nucleotides and effectors as well as regulatory proteins) by exposing appropriate binding sites. For most of these domains, low molecular weight ligands have been identified that either activate or inhibit signal transduction. These ligands include short peptides derived from receptors, G protein subunits and effectors, mastoparan and related insect venoms, modified guanine nucleotides, suramin analogues and amphiphilic cations. Because compounds that act on G proteins may be endowed with new forms of selectivity, we propose that G protein subunits may therefore be considered as potential drug targets.
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页码:257 / 270
页数:13
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