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Published April 12, 2023 | public
Journal Article

Predicted Three-Dimensional Structure of the GCR1 Putative GPCR in Arabidopsis thaliana and Its Binding to Abscisic Acid and Gibberellin A1

Abstract

GCR1 has been proposed as a plant analogue to animal G-protein-coupled receptors that can promote or regulate several physiological processes by binding different phytohormones. For instance, abscisic acid (ABA) and gibberellin A1 (GA1) have been shown to promote or regulate germination and flowering, root elongation, dormancy, and biotic and abiotic stresses, among others. They may act through binding to GCR1, which would put GCR1 at the heart of key signaling processes of agronomic importance. Unfortunately, this GPCR function has yet to be fully validated due to the lack of an X-ray or cryo-EM 3D atomistic structure for GCR1. Here, we used the primary sequence data from Arabidopsis thaliana and the GEnSeMBLE complete sampling method to examine 13 trillion possible packings of the 7 transmembrane helical domains corresponding to GCR1 to downselect an ensemble of 25 configurations likely to be accessible to the binding of ABA or GA1. We then predicted the best binding sites and energies for both phytohormones to the best GCR1 configurations. To provide the basis for the experimental validation of our predicted ligand-GCR1 structures, we identify several mutations that should improve or weaken the interactions. Such validations could help establish the physiological role of GCR1 in plants.

Additional Information

© 2023 American Chemical Society. P.M.H. was partially funded by the OMICAS alliance. A.J.-B. and C.A.A. thank the OMICAS alliance members (the OMICAS program acronym stands for "In-silico Multiscale Optimization of Sustainable Agricultural Crops", a member of the Scientific Colombia Ecosystem, sponsored by the World Bank), the Colombian Ministries of Science, Technology and Innovation (Minciencias), Education, Industry and Tourism, and the ICETEX (project I.D. FP44842-217-2018). S.-K.K. and W.A.G. received support from NIH (R01HL155532). The authors declare no competing financial interest.

Additional details

Created:
August 20, 2023
Modified:
October 20, 2023