Abstract
AbstractBrassinosteroids (BRs) are essential phytohormones which bind to the plant receptor, BRI1, to regulate various physiological processes. The molecular mechanism of the perception of BRs by the ectodomain of BRI1 remains not fully understood. It also remains elusive why a substantial difference in biological activity exists between the BRs. In this work, we study the binding mechanisms of the two most bioactive BRs, brassinolide (BLD) and castasterone (CAT) using molecular dynamics simulations. We report free energy landscapes of the binding processes of both ligands as well as detailed ligand binding pathways. Our results suggest that CAT has lower binding affinity compared to BLD due to its inability to form hydrogen bonding interactions with a tyrosine residue in the island domain of BRI1. We uncover a conserved non-productive binding state for both BLD and CAT, which is more stable for CAT and may further contribute to the bioactivity difference. Finally, we validate past observations about the conformational restructuring and ordering of the island domain upon BLD binding. Overall, this study provides new insights into the fundamental mechanism of the perception of two most bioactive BRs, which may create new avenues for genetic and agrochemical control of their signaling cascade.
Publisher
Cold Spring Harbor Laboratory