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      A structural model of a Ras–Raf signalosome

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          Abstract

          <p class="first" id="d4705328e267">The protein K-Ras functions as a molecular switch in signaling pathways regulating cell growth. In the human mitogen-activated protein kinase (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 guanosine triphosphate-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 and around the helical assembly. The resulting Ras-Raf signalosome model offers an explanation for a large body of data on MAPK signaling. </p>

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          Journal
          Nature Structural & Molecular Biology
          Nat Struct Mol Biol
          Springer Science and Business Media LLC
          1545-9993
          1545-9985
          October 2021
          October 08 2021
          October 2021
          : 28
          : 10
          : 847-857
          Article
          10.1038/s41594-021-00667-6
          8643099
          34625747
          3b3bd57e-83a2-4a90-8b25-50e0684c8026
          © 2021

          https://www.springer.com/tdm

          https://www.springer.com/tdm

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