Molecular analysis of GCN3, a translational activator of GCN4: evidence for posttranslational control of GCN3 regulatory function.

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Mol Cell Biol. 1988 November; 8(11): 4808-4820

Molecular analysis of GCN3, a translational activator of GCN4: evidence for posttranslational control of GCN3 regulatory function.

E M Hannig and A G Hinnebusch

Laboratory of Molecular Genetics, National Institute of Child Health and Human Development, Bethesda, Maryland 20892.

ABSTRACT

GCN4 encodes a transcriptional activator of amino acid biosyntheticgenes in Saccharomyces cerevisiae. The GCN3 product is a positiveregulator required for increased synthesis of GCN4 protein inamino acid-starved cells. GCN3 appears to act indirectly byantagonizing GCD-encoded negative regulators of GCN4 expressionunder starvation conditions; however, GCN3 can also suppressthe effects of gcd12 mutations under nonstarvation conditions.These results imply that the GCN3 product can promote eitherrepression or activation of GCN4 expression depending on aminoacid availability. We present a complete physical descriptionof the GCN3 gene and its transcript, plus measurements of GCN3expression at the transcriptional and translational levels underdifferent growth conditions. GCN3 encodes a 305-amino-acid polypeptidewith no significant homology to any other known protein sequence.GCN3 mRNA contains no leader AUG codons, and no potential GCN4binding sites were found in GCN3 5' noncoding DNA. In accordwith the absence of these regulatory sequences found at othergenes in the general control system, GCN3 mRNA and a GCN3-lacZfusion enzyme are present at similar levels under both starvationand nonstarvation conditions. These data suggest that modulationof GCN3 regulatory function in response to amino acid availabilityoccurs posttranslationally. A gcn3 deletion leads to unconditionallethality in a gcd1-101 mutant, supporting the idea that GCN3is expressed under normal growth conditions and cooperates withthe GCD1 product under these circumstances to carry out an essentialcellular function. We describe a point mutation that adds threeamino acids to the carboxyl terminus of GCN3, which inactivatesits positive regulatory function required under starvation conditionswithout impairing its ability to promote functions carried outby GCD12 under nonstarvation conditions.

Mol Cell Biol. 1988 November; 8(11): 4808-4820

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