Raf promotes dimerization of the Ras G-domain with increased allosteric connections.
Morgan R PackerJillian A ParkerJean K ChungZhen-Lu LiYoung Kwang LeeTrinity CookisHugo GuterresSteven AlvarezMd Amin HossainDaniel P DonnellyJeffery N AgarLee MakowskiMatthias BuckJay T GrovesCarla MattosPublished in: Proceedings of the National Academy of Sciences of the United States of America (2021)
Ras dimerization is critical for Raf activation. Here we show that the Ras binding domain of Raf (Raf-RBD) induces robust Ras dimerization at low surface densities on supported lipid bilayers and, to a lesser extent, in solution as observed by size exclusion chromatography and confirmed by SAXS. Community network analysis based on molecular dynamics simulations shows robust allosteric connections linking the two Raf-RBD D113 residues located in the Galectin scaffold protein binding site of each Raf-RBD molecule and 85 Å apart on opposite ends of the dimer complex. Our results suggest that Raf-RBD binding and Ras dimerization are concerted events that lead to a high-affinity signaling complex at the membrane that we propose is an essential unit in the macromolecular assembly of higher order Ras/Raf/Galectin complexes important for signaling through the Ras/Raf/MEK/ERK pathway.