PT - JOURNAL ARTICLE AU - Richoo B Davis AU - Neah Likhite AU - Christopher A Jackson AU - Tao Liu AU - Michael C Yu TI - Robust repression of tRNA gene transcription during stress requires protein arginine methylation AID - 10.26508/lsa.201800261 DP - 2019 Jun 01 TA - Life Science Alliance PG - e201800261 VI - 2 IP - 3 4099 - https://www.life-science-alliance.org/content/2/3/e201800261.short 4100 - https://www.life-science-alliance.org/content/2/3/e201800261.full SO - Life Sci. Alliance2019 Jun 01; 2 AB - Protein arginine methylation is an important means by which protein function can be regulated. In the budding yeast, this modification is catalyzed by the major protein arginine methyltransferase Hmt1. Here, we provide evidence that the Hmt1-mediated methylation of Rpc31, a subunit of RNA polymerase III, plays context-dependent roles in tRNA gene transcription: under conditions optimal for growth, it positively regulates tRNA gene transcription, and in the setting of stress, it promotes robust transcriptional repression. In the context of stress, methylation of Rpc31 allows for its optimal interaction with RNA polymerase III global repressor Maf1. Interestingly, mammalian Hmt1 homologue is able to methylate one of Rpc31’s human homologue, RPC32β, but not its paralogue, RPC32α. Our data led us to propose an efficient model whereby protein arginine methylation facilitates metabolic economy and coordinates protein-synthetic capacity.