Activity-dependent Reversible Inactivation of the General Amino Acid Permease

April L. Risinger, Natalie E. Cain, Esther J. Chen,* and Chris A. Kaiser

Department of Biology, Massachusetts Institute of Technology, Cambridge, MA 02139

Monitoring Editor: David Drubin

The general amino acid permease,Gap1p, of S. cerevisiae transports all naturally occurring aminoacids into yeast cells for use as a nitrogen source. Previousstudies have shown that a nonubiquitinateable form of the permease,Gap1p^K9R,K16R, is constitutively localized to the plasma membrane.Here, we report that amino acid transport activity of Gap1p^K9R,K16Rcan be rapidly and reversibly inactivated at the plasma membraneby the presence of amino acid mixtures. Surprisingly, we alsofind that addition of most single amino acids is lethal to Gap1p^K9R,K16Rexpressing cells, whereas mixtures of amino acids are less toxic.This toxicity appears to be the consequence of uptake of unusuallylarge quantities of a single amino acid. Exploiting this toxicity,we isolated gap1 alleles deficient in transport of a subsetof amino acids. Using these mutations, we show that Gap1p inactivationat the plasma membrane does not depend on the presence of eitherextracellular or intracellular amino acids, but does requireactive amino acid transport by Gap1p. Together, our findingsuncover a new mechanism for inhibition of permease activityin response to elevated amino acid levels and provide a physiologicalexplanation for the stringent regulation of Gap1p activity inresponse to amino acids.

^*Present address: Department of Biological Sciences, Stanford University, Stanford, CA 94305-5020.

Address correspondence to: Chris A. Kaiser (ckaiser{at}mit.edu)

This article has been cited by other articles:

A. L. Risinger and C. A. Kaiser
Different Ubiquitin Signals Act at the Golgi and Plasma Membrane to Direct GAP1 Trafficking
Mol. Biol. Cell, July 1, 2008; 19(7): 2962 - 2972.
[Abstract] [Full Text] [PDF]