期刊
JOURNAL OF THE AMERICAN CHEMICAL SOCIETY
卷 135, 期 9, 页码 3367-3370出版社
AMER CHEMICAL SOC
DOI: 10.1021/ja312508w
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资金
- Cancer Research Society (Canada) Canadian Cancer Society Research Institute [2010-700494]
- Canada Foundation for Innovation (CFI)
- CFI under Compute Canada
- Government of Ontario
- Ontario Research Fund - Research Excellence
- University of Toronto
Like most Ras superfamily proteins, the GTPase domain of Ras homologue enriched in brain (Rheb) is tethered to cellular membranes through a prenylated cysteine in a flexible C-terminal region; however, little is known about how Rheb or other GTPases interact with the membrane or how this environment may affect their GTPase functions. We used NMR methods to characterize Rheb tethered to nanodiscs, monodisperse protein-encapsulated lipid bilayers with a diameter of 10 nm. Membrane conjugation markedly reduced the rate of intrinsic nucleotide exchange, while GTP hydrolysis was unchanged. NMR measurements revealed that the GTPase domain interacts transiently with the surface of the bilayer in two distinct preferred orientations, which are determined by the bound nucleotide. We propose models of membrane-dependent signal regulation by Rheb that shed light on previously unexplained in vivo properties of this GTPase. The study presented provides a general approach for direct experimental investigation of membrane-dependent properties of other Ras-superfamily GTPases.
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