AI Article Synopsis

  • Elevated reactive oxygen species (ROS) from oxidative stress can damage biomolecules, with RNA being more susceptible to oxidative damage than DNA, particularly ribosomal RNA (rRNA).
  • A genome-wide analysis using 8-oxo-guanosine immunoprecipitation reveals that rRNA is a significant target of oxidative nucleobase damage by ROS, affecting ribosome function.
  • Specific oxidized nucleobases within the ribosome's catalytic center have varied effects, where some are more tolerant to oxidation while others severely disrupt protein synthesis by inhibiting parts of the ribosomal elongation cycle.

Article Abstract

Intracellular levels of reactive oxygen species (ROS) increase as a consequence of oxidative stress and represent a major source of damage to biomolecules. Due to its high cellular abundance RNA is more frequently the target for oxidative damage than DNA. Nevertheless the functional consequences of damage on stable RNA are poorly understood. Using a genome-wide approach, based on 8-oxo-guanosine immunoprecipitation, we present evidence that the most abundant non-coding RNA in a cell, the ribosomal RNA (rRNA), is target for oxidative nucleobase damage by ROS. Subjecting ribosomes to oxidative stress, we demonstrate that oxidized 23S rRNA inhibits the ribosome during protein biosynthesis. Placing single oxidized nucleobases at specific position within the ribosome's catalytic center by atomic mutagenesis resulted in markedly different functional outcomes. While some active site nucleobases tolerated oxidative damage well, oxidation at others had detrimental effects on protein synthesis by inhibiting different sub-steps of the ribosomal elongation cycle. Our data provide molecular insight into the biological consequences of RNA oxidation in one of the most central cellular enzymes and reveal mechanistic insight on the role of individual active site nucleobases during translation.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5829716PMC
http://dx.doi.org/10.1093/nar/gkx1308DOI Listing

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