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MTERF4 regulates translation by targeting the methyltransferase NSUN4 to the mammalian mitochondrial ribosome.

Authors
Cámara, Y | Asin-Cayuela, J | Park, CB  | Metodiev, MD | Shi, Y | Ruzzenente, B | Kukat, C | Habermann, B | Wibom, R | Hultenby, K | Franz, T | Erdjument-Bromage, H | Tempst, P | Hallberg, BM | Gustafsson, CM | Larsson, NG
Citation
Cell metabolism, 13(5). : 527-539, 2011
Journal Title
Cell metabolism
ISSN
1550-41311932-7420
Abstract
Precise control of mitochondrial DNA gene expression is critical for regulation of oxidative phosphorylation capacity in mammals. The MTERF protein family plays a key role in this process, and its members have been implicated in regulation of transcription initiation and site-specific transcription termination. We now demonstrate that a member of this family, MTERF4, directly controls mitochondrial ribosomal biogenesis and translation. MTERF4 forms a stoichiometric complex with the ribosomal RNA methyltransferase NSUN4 and is necessary for recruitment of this factor to the large ribosomal subunit. Loss of MTERF4 leads to defective ribosomal assembly and a drastic reduction in translation. Our results thus show that MTERF4 is an important regulator of translation in mammalian mitochondria.
MeSH

DOI
10.1016/j.cmet.2011.04.002
PMID
21531335
Appears in Collections:
Journal Papers > School of Medicine / Graduate School of Medicine > Physiology
Ajou Authors
박, 찬배
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