Abstract

Mitochondrial DNA (mtDNA) is inherited as a protein–DNA complex (the nucleoid). We show that activation of the general amino acid response pathway in ⁺ and ^- petite cells results in an increased number of nucleoids without an increase in mtDNA copy number. In ^- cells, activation of the general amino acid response pathway results in increased intramolecular recombination between tandemly repeated sequences of ^- mtDNA to produce small, circular oligomers that are packaged into individual nucleoids, resulting in an 10-fold increase in nucleoid number. The parsing of mtDNA into nucleoids due to general amino acid control requires Ilv5p, a mitochondrial protein that also functions in branched chain amino acid biosynthesis, and one or more factors required for mtDNA recombination. Two additional proteins known to function in mtDNA recombination, Abf2p and Mgt1p, are also required for parsing mtDNA into a larger number of nucleoids, although expression of these proteins is not under general amino acid control. Increased nucleoid number leads to increased mtDNA transmission, suggesting a mechanism to enhance mtDNA inheritance under amino acid starvation conditions.