GTPBP8 plays a role in mitoribosome formation in human mitochondria
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Published:2024-07-05
Issue:1
Volume:15
Page:
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ISSN:2041-1723
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Container-title:Nature Communications
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language:en
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Short-container-title:Nat Commun
Author:
Cipullo Miriam, Valentín Gesé Genís, Gopalakrishna ShreekaraORCID, Krueger AnnikaORCID, Lobo Vivian, Pirozhkova Maria A., Marks James, Páleníková PetraORCID, Shiriaev Dmitrii, Liu YongORCID, Misic Jelena, Cai Yu, Nguyen Minh Duc, Abdelbagi AbubakarORCID, Li XinpingORCID, Minczuk MichalORCID, Hafner MarkusORCID, Benhalevy DanielORCID, Sarshad Aishe A.ORCID, Atanassov IlianORCID, Hällberg B. MartinORCID, Rorbach JoannaORCID
Abstract
AbstractMitochondrial gene expression relies on mitoribosomes to translate mitochondrial mRNAs. The biogenesis of mitoribosomes is an intricate process involving multiple assembly factors. Among these factors, GTP-binding proteins (GTPBPs) play important roles. In bacterial systems, numerous GTPBPs are required for ribosome subunit maturation, with EngB being a GTPBP involved in the ribosomal large subunit assembly. In this study, we focus on exploring the function of GTPBP8, the human homolog of EngB. We find that ablation of GTPBP8 leads to the inhibition of mitochondrial translation, resulting in significant impairment of oxidative phosphorylation. Structural analysis of mitoribosomes from GTPBP8 knock-out cells shows the accumulation of mitoribosomal large subunit assembly intermediates that are incapable of forming functional monosomes. Furthermore, fPAR-CLIP analysis reveals that GTPBP8 is an RNA-binding protein that interacts specifically with the mitochondrial ribosome large subunit 16 S rRNA. Our study highlights the role of GTPBP8 as a component of the mitochondrial gene expression machinery involved in mitochondrial large subunit maturation.
Publisher
Springer Science and Business Media LLC
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