Interaction of nucleoside diphosphate kinase B with heterotrimeric G protein βγ dimers: consequences on G protein activation and stability

被引:0
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作者
Thomas Wieland
机构
[1] Universität Heidelberg,Institut für Experimentelle und Klinische Pharmakologie und Toxikologie, Medizinische Fakultät Mannheim
关键词
Heterotrimeric G proteins; Nucleoside diphosphate kinase; nm23-H2; Gβγ dimers; Signal transduction;
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摘要
It is generally accepted that G protein coupled receptors (GPCR) activate heterotrimeric G proteins by inducing a GDP/GTP exchange at the G protein α subunit. In addition, the transfer of high energetic phosphate by nucleoside diphosphate kinase (NDPK) and/or the β subunit of G proteins (Gβ) can induce G protein activation. Recent evidence suggests that the NDPK isoform B (NDPK B) forms a complex with Gβγ dimers. In this complex, NDPK B acts as a protein histidine kinase phosphorylating Gβ at histidine residue 266 (His266). The high energetic phosphoamidate bond on His266 allows for a phosphate transfer specifically onto GDP and thus local formation of GTP, which binds to and thereby activates the respective G protein α subunit. Apparently, this process occurs independent of the classical GPCR-induced GDP/GTP exchange at least for members of the Gs and Gi subfamilies of heterotrimeric G proteins. By using a mutant of Gβ1 in which His266 was replaced by Leu, it was recently demonstrated that NDPK B/Gβγ-mediated Gs activation contributes by about 50% to basal cAMP formation and contractility in rat cardiac myocytes. Besides its apparent role in G protein activation, the complex formation of NDPK B with Gβγ dimers might be essential for G protein stability. Depletion of either the NDPK B orthologue or Gβ1 isoforms in zebrafish embryos led to a similar phenotype displaying contractile dysfunction in the heart accompanied by a complete loss of heterotrimeric G protein expression. In conclusion, the interaction of NDKP B with Gβγ dimers might play an important role in signal transduction, and alterations in this novel pathway might be of pathophysiological importance.
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页码:373 / 383
页数:10
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