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Publication : Cardiolipin is required for membrane docking of mitochondrial ribosomes and protein synthesis.

First Author  Lee RG Year  2020
Journal  J Cell Sci Volume  133
Issue  14 PubMed ID  32576663
Mgi Jnum  J:292652 Mgi Id  MGI:6448828
Doi  10.1242/jcs.240374 Citation  Lee RG, et al. (2020) Cardiolipin is required for membrane docking of mitochondrial ribosomes and protein synthesis. J Cell Sci 133(14):jcs240374
abstractText  The mitochondrial inner membrane contains a unique phospholipid known as cardiolipin (CL), which stabilises the protein complexes embedded in the membrane and supports its overall structure. Recent evidence indicates that the mitochondrial ribosome may associate with the inner membrane to facilitate co-translational insertion of the hydrophobic oxidative phosphorylation (OXPHOS) proteins into the inner membrane. We generated three mutant knockout cell lines for the CL biosynthesis gene Crls1 to investigate the effects of CL loss on mitochondrial protein synthesis. Reduced CL levels caused altered mitochondrial morphology and transcriptome-wide changes that were accompanied by uncoordinated mitochondrial translation rates and impaired respiratory chain supercomplex formation. Aberrant protein synthesis was caused by impaired formation and distribution of mitochondrial ribosomes. Reduction or loss of CL resulted in divergent mitochondrial and endoplasmic reticulum stress responses. We show that CL is required to stabilise the interaction of the mitochondrial ribosome with the membrane via its association with OXA1 (also known as OXA1L) during active translation. This interaction facilitates insertion of newly synthesised mitochondrial proteins into the inner membrane and stabilises the respiratory supercomplexes.
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