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Protein & Peptide Letters

Editor-in-Chief

ISSN (Print): 0929-8665
ISSN (Online): 1875-5305

Local Flexibility Facilitates Oxidization of Buried Methionine Residues

Author(s): Kuiran Xu, Vladimir N. Uversky and Bin Xue

Volume 19, Issue 6, 2012

Page: [688 - 697] Pages: 10

DOI: 10.2174/092986612800494084

Price: $65

Abstract

In proteins, all amino acid residues are susceptible to oxidation by various reactive oxygen species (ROS), with methionine and cysteine residues being particularly sensitive to oxidation. Methionine oxidation is known to lead to destabilization and inactivation of proteins, and oxidatively modified proteins can accumulate during aging, oxidative stress, and in various age-related diseases. Although the efficiency of a given methionine oxidation can depend on its solvent accessibility (evaluated from a protein structure as the accessible surface area of the corresponding methionine residue), many experimental results on oxidation rate and oxidation sites cannot be unequivocally explained by the methionine solvent accessible surface area alone. In order to explore other possible mechanisms, we analyzed a set of seventy-one oxidized methionines contained in thirty-one proteins by various bioinformatics tools. In which, 41% of the methionines are exposed, 15% are buried but with various degree of flexibility, and the rest 44% are buried and structured. Buried but highly flexible methionines can be oxidized. Buried and less flexible methionines can acquire additional local structural flexibility from flanking regions to facilitate the oxidation. Oxidation of buried and structured methionine can also be promoted by the oxidation of neighboring methionine that is more exposed and/or flexible. Our data are consistent with the hypothesis that protein structural flexibility represents another important factor favoring the oxidation process.

Keywords: Bioinformatics, Disorder score, Flexibility, Intrinsic disorder, Methionine oxidation, Solvent accessible surface area, Reactive Oxygen Species (ROS), neurodegenerative diseases, atherosclerosis, muscular dystrophy, oxidized bio-molecules, methionine

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