AI Article Synopsis

  • Many inflammatory diseases are linked to oxidative damage, which alters proteins and influences cell function and disease progression.
  • Oxidized proteins may serve as biomarkers for these diseases, but identifying specific modifications requires advanced techniques like tandem mass spectrometry.
  • The review discusses the strengths and weaknesses of various methods for detecting oxidatively modified proteins, highlighting recent advancements and challenges in accurately identifying these modifications in the context of disease.

Article Abstract

Many inflammatory diseases have an oxidative aetiology, which leads to oxidative damage to biomolecules, including proteins. It is now increasingly recognized that oxidative post-translational modifications (oxPTMs) of proteins affect cell signalling and behaviour, and can contribute to pathology. Moreover, oxidized proteins have potential as biomarkers for inflammatory diseases. Although many assays for generic protein oxidation and breakdown products of protein oxidation are available, only advanced tandem mass spectrometry approaches have the power to localize specific oxPTMs in identified proteins. While much work has been carried out using untargeted or discovery mass spectrometry approaches, identification of oxPTMs in disease has benefitted from the development of sophisticated targeted or semi-targeted scanning routines, combined with chemical labeling and enrichment approaches. Nevertheless, many potential pitfalls exist which can result in incorrect identifications. This review explains the limitations, advantages and challenges of all of these approaches to detecting oxidatively modified proteins, and provides an update on recent literature in which they have been used to detect and quantify protein oxidation in disease.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4496678PMC
http://dx.doi.org/10.3390/biom5020378DOI Listing

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