Role of the histone domain in the autoinhibition and activation of the Ras activator Son of Sevenless
TLDR
The results indicate that the histone domain and the DH-PH unit are conformationally coupled, and that the simultaneous engagement of the membrane by a PH domain PIP2-binding interaction and electrostatic interactions between a conserved positively charged patch on the hist onedomain and the negatively charged membrane coincides with a productive reorientation of SOS at the membrane and increased accessibility of both Ras binding sites on SOS.Abstract:
Membrane-bound Ras is activated by translocation of the Son of Sevenless (SOS) protein to the plasma membrane. SOS is inactive unless Ras is bound to an allosteric site on SOS, and the Dbl homology (DH) and Pleckstrin homology (PH) domains of SOS (the DH-PH unit) block allosteric Ras binding. We showed previously that the activity of SOS at the membrane increases with the density of PIP2 and the local concentration of Ras-GTP, which synergize to release the DH-PH unit. Here we present a new crystal structure of SOS that contains the N-terminal histone domain in addition to the DH-PH unit and the catalytic unit (SOSHDFC, residues 1–1049). The structure reveals that the histone domain plays a dual role in occluding the allosteric site and in stabilizing the autoinhibitory conformation of the DH-PH unit. Additional insight is provided by kinetic analysis of the activation of membrane-bound Ras by mutant forms of SOS that contain mutations in the histone and the PH domains (E108K, C441Y, and E433K) that are associated with Noonan syndrome, a disease caused by hyperactive Ras signaling. Our results indicate that the histone domain and the DH-PH unit are conformationally coupled, and that the simultaneous engagement of the membrane by a PH domain PIP2-binding interaction and electrostatic interactions between a conserved positively charged patch on the histone domain and the negatively charged membrane coincides with a productive reorientation of SOS at the membrane and increased accessibility of both Ras binding sites on SOS.read more
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Journal ArticleDOI
Regulation of Small GTPases by GEFs, GAPs, and GDIs
TL;DR: An overview of the current knowledge of the many facets of small GTPase regulation is presented, including multilayered autoinhibition with stepwise release, feedback loops mediated by the activated GTPases, feed-forward signaling flow between regulators and effectors, and a phosphorylation code for RhoGDIs.
Journal Article
Gain-of-function SOS1 mutations cause a distinctive form of noonan syndrome
Marco Tartaglia,Len A. Pennacchio,Len A. Pennacchio,Chen Zhao,Kamlesh K Yadav,Valentina Fodale,Anna Sarkozy,Anna Sarkozy,Bhaswati Pandit,Kimihiko Oishi,Simone Martinelli,Wendy Schackwitz,Wendy Schackwitz,Anna Ustaszewska,Joel Martin,Joel Martin,James Bristow,James Bristow,Claudio Carta,Francesca Romana Lepri,Francesca Romana Lepri,Cinzia Neri,Cinzia Neri,Isabella Vasta,Kate Gibson,Cynthia J. Curry,Juan Pedro López Siguero,Maria Cristina Digilio,Giuseppe Zampino,Bruno Dallapiccola,Bruno Dallapiccola,Dafna Bar-Sagi,Bruce D. Gelb +32 more
TL;DR: It is reported that 22 of 129 individuals with Noonan syndrome without PTPN11 or KRAS mutation have missense mutations in SOS1, which encodes a RAS-specific guanine nucleotide exchange factor, and this finding defines a new mechanism by which upregulation of the RAS pathway can profoundly change human development.
Journal ArticleDOI
Molecular mechanisms in signal transduction at the membrane
Jay T. Groves,John Kuriyan +1 more
TL;DR: This review discusses recent mechanistic insights into three signaling systems—Ras activation, Ephrin signaling and the control of actin nucleation—where the active role of membrane components is now appreciated and for which experimentation on the membrane is required for further understanding.
Journal ArticleDOI
A molecular assembly phase transition and kinetic proofreading modulate Ras activation by SOS.
William Y. C. Huang,Steven Alvarez,Yasushi Kondo,Yasushi Kondo,Young Kwang Lee,Jean K. Chung,Hiu Yue Monatrice Lam,Kabir H. Biswas,John Kuriyan,Jay T. Groves,Jay T. Groves,Jay T. Groves +11 more
TL;DR: A single-molecule assay is designed to resolve the time between initial receptor-mediated membrane recruitment and the initiation of GEF activity of individual SOS molecules on microarrays of Ras-functionalized supported membranes, establish a basis for kinetic proofreading in the receptor- mediated activation of Ras, and shows how such condensates function in actin assembly or in a Ras signaling pathway.
Journal ArticleDOI
NMR-based functional profiling of RASopathies and oncogenic RAS mutations.
TL;DR: The NMR method presents a precise and robust measure of RAS activity, providing mechanistic insights that facilitate discovery of therapeutics targeted against the RAS signaling network.
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The structural basis of the activation of Ras by Sos
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Marco Tartaglia,Len A. Pennacchio,Len A. Pennacchio,Chen Zhao,Kamlesh K Yadav,Valentina Fodale,Anna Sarkozy,Anna Sarkozy,Bhaswati Pandit,Kimihiko Oishi,Simone Martinelli,Wendy Schackwitz,Wendy Schackwitz,Anna Ustaszewska,Joel Martin,Joel Martin,James Bristow,James Bristow,Claudio Carta,Francesca Romana Lepri,Francesca Romana Lepri,Cinzia Neri,Cinzia Neri,Isabella Vasta,Kate Gibson,Cynthia J. Curry,Juan Pedro López Siguero,Maria Cristina Digilio,Giuseppe Zampino,Bruno Dallapiccola,Bruno Dallapiccola,Dafna Bar-Sagi,Bruce D. Gelb +32 more