The FASTK family proteins fine-tune mitochondrial RNA processing

生物 核糖核酸 遗传学 转移RNA RNA编辑 细胞生物学 转录组 线粒体 基因 基因表达
作者
Akira Ohkubo,Lindsey Van Haute,Danielle L. Rudler,Maike Stentenbach,Florian Steiner,Oliver Rackham,Michal Minczuk,Aleksandra Filipovska,Jean‐Claude Martinou
出处
期刊:PLOS Genetics [Public Library of Science]
卷期号:17 (11): e1009873-e1009873 被引量:33
标识
DOI:10.1371/journal.pgen.1009873
摘要

Transcription of the human mitochondrial genome and correct processing of the two long polycistronic transcripts are crucial for oxidative phosphorylation. According to the tRNA punctuation model, nucleolytic processing of these large precursor transcripts occurs mainly through the excision of the tRNAs that flank most rRNAs and mRNAs. However, some mRNAs are not punctuated by tRNAs, and it remains largely unknown how these non-canonical junctions are resolved. The FASTK family proteins are emerging as key players in non-canonical RNA processing. Here, we have generated human cell lines carrying single or combined knockouts of several FASTK family members to investigate their roles in non-canonical RNA processing. The most striking phenotypes were obtained with loss of FASTKD4 and FASTKD5 and with their combined double knockout. Comprehensive mitochondrial transcriptome analyses of these cell lines revealed a defect in processing at several canonical and non-canonical RNA junctions, accompanied by an increase in specific antisense transcripts. Loss of FASTKD5 led to the most severe phenotype with marked defects in mitochondrial translation of key components of the electron transport chain complexes and in oxidative phosphorylation. We reveal that the FASTK protein family members are crucial regulators of non-canonical junction and non-coding mitochondrial RNA processing.

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