Detection of methylation, acetylation and glycosylation of protein residues by monitoring 13C chemical-shift changes: A quantum-chemical study

Post-translational modifications of proteins expand the diversity of the proteome by several orders of magnitude and have a profound effect on several biological processes. Their detection by experimental methods is not free of limitations such as the amount of sample needed or the use of destructiv...

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Main Authors: Pablo G. Garay, Osvaldo A. Martin, Harold A. Scheraga, Jorge A. Vila
Format: Article
Language:English
Published: PeerJ Inc. 2016-07-01
Series:PeerJ
Subjects:
Online Access:https://peerj.com/articles/2253.pdf
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spelling doaj-5bf5b12c40ae48d680b0e5d9b9b1a7e12020-11-24T22:56:06ZengPeerJ Inc.PeerJ2167-83592016-07-014e225310.7717/peerj.2253Detection of methylation, acetylation and glycosylation of protein residues by monitoring 13C chemical-shift changes: A quantum-chemical studyPablo G. Garay0Osvaldo A. Martin1Harold A. Scheraga2Jorge A. Vila3IMASL-CONICET, Universidad Nacional de San Luis, San Luis, ArgentinaIMASL-CONICET, Universidad Nacional de San Luis, San Luis, ArgentinaChemistry and Chemical Biology, Cornell University, Ithaca, NY, USAIMASL-CONICET, Universidad Nacional de San Luis, San Luis, ArgentinaPost-translational modifications of proteins expand the diversity of the proteome by several orders of magnitude and have a profound effect on several biological processes. Their detection by experimental methods is not free of limitations such as the amount of sample needed or the use of destructive procedures to obtain the sample. Certainly, new approaches are needed and, therefore, we explore here the feasibility of using 13C chemical shifts of different nuclei to detect methylation, acetylation and glycosylation of protein residues by monitoring the deviation of the 13C chemical shifts from the expected (mean) experimental value of the non-modified residue. As a proof-of-concept, we used 13C chemical shifts, computed at the DFT-level of theory, to test this hypothesis. Moreover, as a validation test of this approach, we compare our theoretical computations of the 13Cε chemical-shift values against existing experimental data, obtained from NMR spectroscopy, for methylated and acetylated lysine residues with good agreement within ∼1 ppm. Then, further use of this approach to select the most suitable 13C-nucleus, with which to determine other modifications commonly seen, such as methylation of arginine and glycosylation of serine, asparagine and threonine, shows encouraging results.https://peerj.com/articles/2253.pdfPost-translational modificationsMethylationGlycosylationAcetylationProteinGlycan
collection DOAJ
language English
format Article
sources DOAJ
author Pablo G. Garay
Osvaldo A. Martin
Harold A. Scheraga
Jorge A. Vila
spellingShingle Pablo G. Garay
Osvaldo A. Martin
Harold A. Scheraga
Jorge A. Vila
Detection of methylation, acetylation and glycosylation of protein residues by monitoring 13C chemical-shift changes: A quantum-chemical study
PeerJ
Post-translational modifications
Methylation
Glycosylation
Acetylation
Protein
Glycan
author_facet Pablo G. Garay
Osvaldo A. Martin
Harold A. Scheraga
Jorge A. Vila
author_sort Pablo G. Garay
title Detection of methylation, acetylation and glycosylation of protein residues by monitoring 13C chemical-shift changes: A quantum-chemical study
title_short Detection of methylation, acetylation and glycosylation of protein residues by monitoring 13C chemical-shift changes: A quantum-chemical study
title_full Detection of methylation, acetylation and glycosylation of protein residues by monitoring 13C chemical-shift changes: A quantum-chemical study
title_fullStr Detection of methylation, acetylation and glycosylation of protein residues by monitoring 13C chemical-shift changes: A quantum-chemical study
title_full_unstemmed Detection of methylation, acetylation and glycosylation of protein residues by monitoring 13C chemical-shift changes: A quantum-chemical study
title_sort detection of methylation, acetylation and glycosylation of protein residues by monitoring 13c chemical-shift changes: a quantum-chemical study
publisher PeerJ Inc.
series PeerJ
issn 2167-8359
publishDate 2016-07-01
description Post-translational modifications of proteins expand the diversity of the proteome by several orders of magnitude and have a profound effect on several biological processes. Their detection by experimental methods is not free of limitations such as the amount of sample needed or the use of destructive procedures to obtain the sample. Certainly, new approaches are needed and, therefore, we explore here the feasibility of using 13C chemical shifts of different nuclei to detect methylation, acetylation and glycosylation of protein residues by monitoring the deviation of the 13C chemical shifts from the expected (mean) experimental value of the non-modified residue. As a proof-of-concept, we used 13C chemical shifts, computed at the DFT-level of theory, to test this hypothesis. Moreover, as a validation test of this approach, we compare our theoretical computations of the 13Cε chemical-shift values against existing experimental data, obtained from NMR spectroscopy, for methylated and acetylated lysine residues with good agreement within ∼1 ppm. Then, further use of this approach to select the most suitable 13C-nucleus, with which to determine other modifications commonly seen, such as methylation of arginine and glycosylation of serine, asparagine and threonine, shows encouraging results.
topic Post-translational modifications
Methylation
Glycosylation
Acetylation
Protein
Glycan
url https://peerj.com/articles/2253.pdf
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