Effects of farnesylcysteine analogs on protein carboxyl methylation and signal transduction.

  1. C Volker,
  2. R A Miller,
  3. W R McCleary,
  4. A Rao,
  5. M Poenie,
  6. J M Backer and
  7. J B Stock
  1. Department of Molecular Biology, Princeton University, New Jersey 08544-1014.

    Abstract

    Several proteins associated with signal transduction in eukaryotes are carboxyl methylated at COOH-terminal S-farnesylcysteine residues. These include members of the Ras superfamily and gamma-subunits of heterotrimeric G-proteins. The enzymes that catalyze the carboxyl methylation reaction also methylate small molecules such as N-acetyl-S-trans, trans-farnesyl-L-cysteine (AFC). AFC inhibits carboxyl methylation of p21ras and related proteins both in vitro and in vivo. Saturating concentrations of AFC cause a greater than 80% inhibition of chemotactic responses of mouse peritoneal macrophages. Our results suggest that carboxyl methylation may play a role in the regulation of receptor-mediated signal transduction processes in eukaryotic cells.

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    1. November 15, 1991 The Journal of Biological Chemistry, 266, 21515-21522.
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