Selective Inhibition of <i>ras</i> -Dependent Transformation by a Farnesyltransferase Inhibitor

Nancy E. Kohl; Scott D. Mosser; S. J. DESOLMS; Elizabeth A. Giuliani; David L. Pompliano; Samuel Graham; Robert L. Smith; Edward M. Scolnick; Allen Oliff; W. Wayt Gibbs

doi:10.1126/science.8316833

Selective Inhibition of <i>ras</i> -Dependent Transformation by a Farnesyltransferase Inhibitor

Nancy E. Kohl(United States Military Academy), Scott D. Mosser(United States Military Academy), S. J. DESOLMS(United States Military Academy), Elizabeth A. Giuliani(United States Military Academy), David L. Pompliano(United States Military Academy), Samuel Graham(United States Military Academy), Robert L. Smith(United States Military Academy), Edward M. Scolnick(United States Military Academy), Allen Oliff(United States Military Academy), W. Wayt Gibbs(United States Military Academy)

Science

June 25, 1993

10.1126/science.8316833

Cited by 582

Abstract

To acquire transforming potential, the precursor of the Ras oncoprotein must undergo farnesylation of the cysteine residue located in a carboxyl-terminal tetrapeptide. Inhibitors of the enzyme that catalyzes this modification, farnesyl protein transferase (FPTase), have therefore been suggested as anticancer agents for tumors in which Ras contributes to transformation. The tetrapeptide analog L-731,735 is a potent and selective inhibitor of FPTase in vitro. A prodrug of this compound, L-731,734, inhibited Ras processing in cells transformed with v-ras. L-731,734 decreased the ability of v-ras-transformed cells to form colonies in soft agar but had no effect on the efficiency of colony formation of cells transformed by either the v-raf or v-mos oncogenes. The results demonstrate selective inhibition of ras-dependent cell transformation with a synthetic organic inhibitor of FPTase.

Related Papers

No related papers found

Powered by citation graph analysis