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Cell Growth and Development

Rap2 as a Slowly Responding Molecular Switch in the Rap1 Signaling Cascade

, , , , , , , , & show all
Pages 6074-6083 | Received 29 Dec 1999, Accepted 08 May 2000, Published online: 28 Mar 2023
 

Abstract

Rap2 is a member of the Ras family of GTPases and exhibits 60% identity to Rap1, but the function and regulation of Rap2 remain obscure. We found that, unlike the other Ras family proteins, the GTP-bound active form exceeded 50% of total Rap2 protein in adherent cells. Guanine nucleotide exchange factors (GEFs) for Rap1, C3G, Epac (or cyclic AMP [cAMP]-GEF), CalDAG-GEFI, PDZ-GEF1, and GFR efficiently increased the level of GTP-Rap2 both in 293T cells and in vitro. GTPase-activating proteins (GAPs) for Rap1, rap1GAPII and SPA-1, stimulated Rap2 GTPase, but with low efficiency. The half-life of GTP-Rap2 was significantly longer than that of GTP-Rap1 in 293T cells, indicating that low sensitivity to GAPs caused a high GTP/GDP ratio on Rap2. Rap2 bound to the Ras-binding domain of Raf and inhibited Ras-dependent activation of Elk1 transcription factor, as did Rap1. The level of GTP-Rap2 in rat 3Y1 fibroblasts was decreased by the expression of v-Src, and expression of a GTPase-deficient Rap2 mutant inhibited v-Src-dependent transformation of 3Y1 cells. Altogether, Rap2 is regulated by a similar set of GEFs and GAPs as Rap1 and functions as a slowly responding molecular switch in the Rap1 signaling cascade.

ACKNOWLEDGMENTS

We thank J. L. Bos, A. Wittinghofer, B. J. Mayer, C. Lenzen, S. Hattori, S. Hirohashi, S. Iwasaka, J. Miyazaki, H. Kitayama, and M. Noda for materials and K. Okuda, N. Otsuka, and F. Ohba for technical assistance.

This work was supported by grants from the Ministry of Health and Welfare; Ministry of Education, Science, Sports and Culture; the Naito Foundation; and the Health Science Foundation, Japan.

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