AI Article Synopsis
- G-protein-coupled receptor kinases (GRKs), specifically GRK5, not only regulate GPCR signaling but also play a critical role in gene transcription by translocating to the nucleus.
- Overexpression of GRK5 leads to increased levels of IkappaB alpha in the nucleus, which inhibits NFkappaB transcriptional activity, whereas knocking down GRK5 yields the opposite effect.
- The interaction between GRK5 and IkappaB alpha is mediated by specific protein domains, and this mechanism may serve as a potential therapeutic target for conditions associated with heightened NFkappaB activity, influencing processes like apoptosis and inflammation.
Article Abstract
G-protein-coupled receptor (GPCR) kinases, GRKs, are known as serine/threonine kinases that regulate GPCR signaling, but recent findings propose functions for these kinases besides receptor desensitization. Indeed, GRK5 can translocate to the nucleus by means of a nuclear localization sequence, suggesting that this kinase regulates transcription events in the nucleus. To evaluate the effect of GRK5-IkappaB alpha interaction on NFkappaB signaling, we induced the overexpression and the knockdown of GRK5 in cell cultures. GRK5 overexpression causes nuclear accumulation of IkappaB alpha, leading to the inhibition of NFkappaB transcriptional activity. Opposite results are achieved by GRK5 knockdown through siRNA. A physical interaction between GRK5 and IkappaB alpha, rather than phosphorylative events, appears as the underlying mechanism. We identify the regulator of gene protein signaling homology domain of GRK5 (RH) and the N-terminal domain of IkappaB alpha as the regions involved in such interaction. To confirm the biological relevance of this mechanism of regulation for NFkappaB, we evaluated the effects of GRK5-RH on NFkappaB-dependent phenotypes. In particular, GRK5-RH overexpression impairs apoptosis protection and cytokine production in vitro and inflammation and tissue regeneration in vivo. Our results reveal an unexpected role for GRK5 in the regulation of NFkappaB transcription activity. Placing these findings in perspective, this mechanism may represent a therapeutic target for all those conditions involving excessive NFkappaB activity.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2584738 | PMC |
| http://dx.doi.org/10.1073/pnas.0804446105 | DOI Listing |
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