A structural model of a Ras-Raf signalosome

Author:

Mysore Venkatesh P.,Zhou Zhi-Wei,Ambrogio Chiara,Li Lianbo,Kapp Jonas N.,Lu Chunya,Wang Qi,Tucker Maxwell R.,Okoro Jeffrey J.,Nagy-Davidescu Gabriela,Bai Xiaochen,Plückthun Andreas,Jänne Pasi A.,Westover Kenneth D.,Shan Yibing,Shaw David E.

Abstract

AbstractThe protein K-Ras functions as a molecular switch in signaling pathways regulating cell growth. In the MAPK pathway, which is implicated in many cancers, multiple K-Ras proteins are thought to assemble at the cell membrane with Ras-effector proteins from the Raf family. Here we propose an atomistic structural model for such an assembly. Our starting point was an asymmetric, GTP-mediated K-Ras dimer model, which we generated using unbiased molecular dynamics simulations and verified with mutagenesis experiments. Adding further K-Ras monomers in a head-to-tail fashion led to a compact helical assembly, a model we validated using electron microscopy and cell-based experiments. This assembly stabilizes K-Ras in its active state and presents composite interfaces to facilitate Raf binding. Guided by existing experimental data, we then positioned C-Raf, the downstream kinase MEK1, and accessory proteins (Galectin-3 and 14-3-3σ) on the helical assembly. The resulting Ras-Raf signalosome model offers an explanation for a large body of data on MAPK signaling.

Publisher

Cold Spring Harbor Laboratory

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