AI Article Synopsis

  • The evolution of mitochondrial information processing pathways shows a shift from mitochondrial-encoded proteins to nuclear-encoded ones, especially in transcription and replication, while mitochondrial translation retains many ancestral features.
  • Recent studies of certain animal phyla, including Cnidaria and Ctenophora, indicate ongoing evolution in mitochondrial translation, particularly among various tRNAs.
  • Findings reveal that the interaction between nuclear and mitochondrial proteins in translation is more complex than previously thought, suggesting that relaxed selection has led to increased evolutionary rates in mitochondrial translational proteins.

Article Abstract

The evolution of mitochondrial information processing pathways, including replication, transcription and translation, is characterized by the gradual replacement of mitochondrial-encoded proteins with nuclear-encoded counterparts of diverse evolutionary origins. Although the ancestral enzymes involved in mitochondrial transcription and replication have been replaced early in eukaryotic evolution, mitochondrial translation is still carried out by an apparatus largely inherited from the α-proteobacterial ancestor. However, variation in the complement of mitochondrial-encoded molecules involved in translation, including transfer RNAs (tRNAs), provides evidence for the ongoing evolution of mitochondrial protein synthesis. Here, we investigate the evolution of the mitochondrial translational machinery using recent genomic and transcriptomic data from animals that have experienced the loss of mt-tRNAs, including phyla Cnidaria and Ctenophora, as well as some representatives of all four classes of Porifera. We focus on four sets of mitochondrial enzymes that directly interact with tRNAs: Aminoacyl-tRNA synthetases, glutamyl-tRNA amidotransferase, tRNA(Ile) lysidine synthetase, and RNase P. Our results support the observation that the fate of nuclear-encoded mitochondrial proteins is influenced by the evolution of molecules encoded in mitochondrial DNA, but in a more complex manner than appreciated previously. The data also suggest that relaxed selection on mitochondrial translation rather than coevolution between mitochondrial and nuclear subunits is responsible for elevated rates of evolution in mitochondrial translational proteins.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4558845PMC
http://dx.doi.org/10.1093/gbe/evv124DOI Listing

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