bims-tricox Biomed News
on Translation, ribosomes and COX
Issue of 2023‒07‒02
three papers selected by
Yash Verma
University of Zurich
  1. Translation termination in human mitochondria - substrate specificity of mitochondrial release factors.
  2. The unfolded protein response of the endoplasmic reticulum supports mitochondrial biogenesis by buffering non-imported proteins.
  3. 35 Years of TFAM Research: Old Protein, New Puzzles.
  1. Biol Chem. 2023 Jun 29.
    Translation termination in human mitochondria - substrate specificity of mitochondrial release factors.
    Franziska Nadler, Ricarda Richter-Dennerlein.
      Mitochondria are the essential players in eukaryotic ATP production by oxidative phosphorylation, which relies on the maintenance and accurate expression of the mitochondrial genome. Even though the basic principles of translation are conserved due to the descendance from a bacterial ancestor, some deviations regarding translation factors as well as mRNA characteristics and the applied genetic code are present in human mitochondria. Together, these features are certain challenges during translation the mitochondrion has to handle. Here, we discuss the current knowledge regarding mitochondrial translation focusing on the termination process and the associated quality control mechanisms. We describe how mtRF1a resembles bacterial RF1 mechanistically and summarize in vitro and recent in vivo data leading to the conclusion of mtRF1a being the major mitochondrial release factor. On the other hand, we discuss the ongoing debate about the function of the second codon-dependent mitochondrial release factor mtRF1 regarding its role as a specialized termination factor. Finally, we link defects in mitochondrial translation termination to the activation of mitochondrial rescue mechanisms highlighting the importance of ribosome-associated quality control for sufficient respiratory function and therefore for human health.
    Keywords:  COX1 translation; mitoribosome rescue; mitoribosome-associated quality control; mtRF1; mtRF1a; non-canonical stop codons
    DOI:  https://doi.org/10.1515/hsz-2023-0127
  2. Mol Biol Cell. 2023 Jun 28. mbcE23050205
    The unfolded protein response of the endoplasmic reticulum supports mitochondrial biogenesis by buffering non-imported proteins.
    Katharina Knöringer, Carina Groh, Lena Krämer, Kevin C Stein, Katja G Hansen, Jannik Zimmermann, Bruce Morgan, Johannes M Herrmann, Judith Frydman, Felix Boos.
      Almost all mitochondrial proteins are synthesized in the cytosol and subsequently targeted to mitochondria. The accumulation of non-imported precursor proteins occurring upon mitochondrial dysfunction can challenge cellular protein homeostasis. Here we show that blocking protein translocation into mitochondria results in the accumulation of mitochondrial membrane proteins at the endoplasmic reticulum, thereby triggering the unfolded protein response (UPRER). Moreover, we find that mitochondrial membrane proteins are also routed to the ER under physiological conditions. The level of ER-resident mitochondrial precursors is enhanced by import defects as well as metabolic stimuli that increase the expression of mitochondrial proteins. Under such conditions, the UPRER is crucial to maintain protein homeostasis and cellular fitness. We propose the ER serves as a physiological buffer zone for those mitochondrial precursors that cannot be immediately imported into mitochondria while engaging the UPRER to adjust the ER proteostasis capacity to the extent of precursor accumulation.
    DOI:  https://doi.org/10.1091/mbc.E23-05-0205
  3. Biology (Basel). 2023 Jun 06. pii: 823. [Epub ahead of print]12(6):
    35 Years of TFAM Research: Old Protein, New Puzzles.
    Natalya Kozhukhar, Mikhail F Alexeyev.
      Transcription Factor A Mitochondrial (TFAM), through its contributions to mtDNA maintenance and expression, is essential for cellular bioenergetics and, therefore, for the very survival of cells. Thirty-five years of research on TFAM structure and function generated a considerable body of experimental evidence, some of which remains to be fully reconciled. Recent advancements allowed an unprecedented glimpse into the structure of TFAM complexed with promoter DNA and TFAM within the open promoter complexes. These novel insights, however, raise new questions about the function of this remarkable protein. In our review, we compile the available literature on TFAM structure and function and provide some critical analysis of the available data.
    Keywords:  mitochondria; mitochondrial DNA; mitochondrial DNA repair; mitochondrial DNA replication; mitochondrial DNA transcription; mitochondrial biogenesis; mitochondrial transcription factor A (TFAM)
    DOI:  https://doi.org/10.3390/biology12060823
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