TY - DATA T1 - Stress-response transcription factors Msn2 and Msn4 couple TORC2-Ypk1 signaling and mitochondrial respiration to ATG8 gene expression and autophagy PY - 2017/12/04 AU - Ariadne Vlahakis AU - Nerea Lopez Muniozguren AU - Ted Powers UR - https://tandf.figshare.com/articles/journal_contribution/Stress-response_transcription_factors_Msn2_and_Msn4_couple_TORC2-Ypk1_signaling_and_mitochondrial_respiration_to_i_ATG8_i_gene_expression_and_autophagy/5662225 DO - 10.6084/m9.figshare.5662225 L4 - https://ndownloader.figshare.com/files/9879922 KW - autophagy KW - electron transport chain (ETC) complexes KW - gene expression KW - mitochondrial respiration KW - signal transduction KW - TOR signaling KW - Ypk1 N2 - Macroautophagy/autophagy is a starvation and stress-induced catabolic process critical for cellular homeostasis and adaptation. Several Atg proteins are involved in the formation of the autophagosome and subsequent degradation of cytoplasmic components, a process termed autophagy flux. Additionally, the expression of several Atg proteins, in particular Atg8, is modulated transcriptionally, yet the regulatory mechanisms involved remain poorly understood. Here we demonstrate that the AGC kinase Ypk1, target of the rapamycin-insensitive TORC2 signaling pathway, controls ATG8 expression by repressing the heterodimeric Zinc-finger transcription factors Msn2 and Msn4. We find that Msn2 and Msn4 promote ATG8 expression downstream of the histone deacetylase complex (HDAC) subunit Ume6, a previously identified negative regulator of ATG8 expression. Moreover, we demonstrate that TORC2-Ypk1 signaling is functionally linked to distinct mitochondrial respiratory complexes. Surprisingly, we find that autophagy flux during amino acid starvation is also dependent upon Msn2-Msn4 activity, revealing a broad role for these transcription factors in the autophagy response. ER -