Abstract

The G-protein regulatory (GPR) motif in AGS3 was recently identified as a region for protein binding to heterotrimeric G-protein alpha subunits. To define the properties of this approximately 20-amino acid motif, we designed a GPR consensus peptide and determined its influence on the activation state of G-protein and receptor coupling to G-protein. The GPR peptide sequence (28 amino acids) encompassed the consensus sequence defined by the four GPR motifs conserved in the family of AGS3 proteins. The GPR consensus peptide effectively prevented the binding of AGS3 to Gialpha1,2 in protein interaction assays, inhibited guanosine 5'-O-(3-thiotriphosphate) binding to Gialpha, and stabilized the GDP-bound conformation of Gialpha. The GPR peptide had little effect on nucleotide binding to Goalpha and brain G-protein indicating selective regulation of Gialpha. Thus, the GPR peptide functions as a guanine nucleotide dissociation inhibitor for Gialpha. The GPR consensus peptide also blocked receptor coupling to Gialphabetagamma indicating that although the AGS3-GPR peptide stabilized the GDP-bound conformation of Gialpha, this conformation of Gialpha(GDP) was not recognized by a G-protein coupled receptor. The AGS3-GPR motif presents an opportunity for selective control of Gialpha- and Gbetagamma-regulated effector systems, and the GPR motif allows for alternative modes of signal input to G-protein signaling systems.

Highlights

  • Stabilization of the GDP-bound Conformation of Gi␣ by a Peptide Derived from the G-protein Regulatory Motif of AGS3*

  • The G-protein regulatory (GPR) consensus peptide blocked receptor coupling to Gi␣␤␥ indicating that the AGS3GPR peptide stabilized the GDP-bound conformation of Gi␣, this conformation of Gi␣GDP was not recognized by a G-protein coupled receptor

  • The AGS3-GPR motif presents an opportunity for selective control of Gi␣- and G␤␥؊regulated effector systems, and the GPR motif allows for alternative modes of signal input to G-protein signaling systems

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Summary

Introduction

Stabilization of the GDP-bound Conformation of Gi␣ by a Peptide Derived from the G-protein Regulatory Motif of AGS3*. The GPR consensus peptide effectively prevented the binding of AGS3 to Gi␣1,2 in protein interaction assays, inhibited guanosine 5؅-O-(3-thiotriphosphate) binding to Gi␣, and stabilized the GDP-bound conformation of Gi␣.

Results
Conclusion
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