Translation initiation of leaderless and polycistronic transcripts in mammalian mitochondria

Remes, Cristina; Kyriakidis, Vasileios; Firth, Andrew E; Zhang, Jingdian; Khawaja, Anas; Atanassov, Ilian; Dopico, Xaquin Castro; Rorbach, Joanna; Cipullo, Miriam; Yukhnovets, Olessya; Pearce, Sarah F; Gopalakrishna, Shreekara; Cooperman, Barry; Dinan, Adam M

doi:10.1093/nar/gkac1233

Journal Article

FZJ-2023-02031

Translation initiation of leaderless and polycistronic transcripts in mammalian mitochondria

Remes, C. (Corresponding author) ; Khawaja, A. (First author) ; Pearce, S. F. ; Dinan, A. M. ; Gopalakrishna, S. ; Cipullo, M. ; Kyriakidis, V. ; Zhang, J. ; Dopico, X. C. ; Yukhnovets, O.FZJ* ; Atanassov, I. ; Firth, A. E. ; Cooperman, B. ; Rorbach, J.

2023
Oxford Univ. Press Oxford

Nucleic acids research 51(2), 891 - 907 (2023) [10.1093/nar/gkac1233]

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Please use a persistent id in citations: http://hdl.handle.net/2128/34449 doi:10.1093/nar/gkac1233

Abstract: The synthesis of mitochondrial OXPHOS complexes is central to cellular metabolism, yet many molecular details of mitochondrial translation remain elusive. It has been commonly held view that translation initiation in human mitochondria proceeded in a manner similar to bacterial systems, with the mitoribosomal small subunit bound to the initiation factors, mtIF2 and mtIF3, along with initiator tRNA and an mRNA. However, unlike in bacteria, most human mitochondrial mRNAs lack 5′ leader sequences that can mediate small subunit binding, raising the question of how leaderless mRNAs are recognized by mitoribosomes. By using novel in vitro mitochondrial translation initiation assays, alongside biochemical and genetic characterization of cellular knockouts of mitochondrial translation factors, we describe unique features of translation initiation in human mitochondria. We show that in vitro, leaderless mRNA transcripts can be loaded directly onto assembled 55S mitoribosomes, but not onto the mitoribosomal small subunit (28S), in a manner that requires initiator fMet-tRNAMet binding. In addition, we demonstrate that in human cells and in vitro, mtIF3 activity is not required for translation of leaderless mitochondrial transcripts but is essential for translation of ATP6 in the case of the bicistronic ATP8/ATP6 transcript. Furthermore, we show that mtIF2 is indispensable for mitochondrial protein synthesis. Our results demonstrate an important evolutionary divergence of the mitochondrial translation system and further our fundamental understanding of a process central to eukaryotic metabolism.

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ddc:570

Contributing Institute(s):

Zelluläre Strukturbiologie (IBI-6)

Research Program(s):

5352 - Understanding the Functionality of Soft Matter and Biomolecular Systems (POF4-535) (POF4-535)

Appears in the scientific report 2023

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Record created 2023-05-09, last modified 2024-06-10

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