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Non-Mitochondrial Aconitase-2 Mediates the Transcription of Nuclear-Encoded Electron Transport Chain Genes in Fission Yeast

Authors
Kim, Ho-JungCho, Soo-YeonJung, Soo-JinCho, Yong-JunRoe, Jung-HyeKim, Kyoung-Dong
Issue Date
Jun-2024
Publisher
Springer Nature
Keywords
Aconitase; Electron transport chain; ETC; Fission yeast; Php complex; Respiration
Citation
Journal of Microbiology
Journal Title
Journal of Microbiology
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/75023
DOI
10.1007/s12275-024-00147-8
ISSN
1225-8873
1976-3794
Abstract
Aconitase-2 (Aco2) is present in the mitochondria, cytosol, and nucleus of fission yeast. To explore its function beyond the well-known role in the mitochondrial tricarboxylic acid (TCA) cycle, we conducted genome-wide profiling using the aco2ΔNLS mutant, which lacks a nuclear localization signal (NLS). The RNA sequencing (RNA-seq) data showed a general downregulation of electron transport chain (ETC) genes in the aco2ΔNLS mutant, except for those in the complex II, leading to a growth defect in respiratory-prone media. Complementation analysis with non-catalytic Aco2 [aco2ΔNLS + aco2(3CS)], where three cysteines were substituted with serine, restored normal growth and typical ETC gene expression. This suggests that Aco2’s catalytic activity is not essential for its role in ETC gene regulation. Our mRNA decay assay indicated that the decrease in ETC gene expression was due to transcriptional regulation rather than changes in mRNA stability. Additionally, we investigated the Php complex’s role in ETC gene regulation and found that ETC genes, except those within complex II, were downregulated in php3Δ and php5Δ strains, similar to the aco2ΔNLS mutant. These findings highlight a novel role for nuclear aconitase in ETC gene regulation and suggest a potential connection between the Php complex and Aco2. © The Author(s), under exclusive licence to Microbiological Society of Korea 2024.
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Kim, Kyoung-Dong
생명공학대학 (시스템생명공학과)
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