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Cell Growth and Development

Three Separable Domains Regulate GTP-Dependent Association of H-ras with the Plasma Membrane

, , , , , & show all
Pages 6799-6810 | Received 08 Apr 2004, Accepted 10 May 2004, Published online: 27 Mar 2023
 

Abstract

The microlocalization of Ras proteins to different microdomains of the plasma membrane is critical for signaling specificity. Here we examine the complex membrane interactions of H-ras with a combination of FRAP on live cells to measure membrane affinity and electron microscopy of intact plasma membrane sheets to spatially map microdomains. We show that three separable forces operate on H-ras at the plasma membrane. The lipid anchor, comprising a processed CAAX motif and two palmitic acid residues, generates one attractive force that provides a high-affinity interaction with lipid rafts. The adjacent hypervariable linker domain provides a second attractive force but for nonraft plasma membrane microdomains. Operating against the attractive interaction of the lipid anchor for lipid rafts is a repulsive force generated by the N-terminal catalytic domain that increases when H-ras is GTP loaded. These observations lead directly to a novel mechanism that explains how H-ras lateral segregation is regulated by activation state: GTP loading decreases H-ras affinity for lipid rafts and allows the hypervariable linker domain to target to nonraft microdomains, the primary site of H-ras signaling.

This work was supported by grants from the National Institutes of Health (GM-066717) and the National Health and Medical Research Council to J.F.H. and R.G.P. I.A.P. is a Royal Society University Research Fellow. Y.I.H. is an incumbent of the Zalman Weinberg Chair in Cell Biology.

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