Warning: Undefined array key "mm" in /www/wwwroot/www.ai-bt.com/si.php on line 10 Deprecated: trim(): Passing null to parameter #1 ($string) of type string is deprecated in /www/wwwroot/www.ai-bt.com/si.php on line 10 Mechanistic insights into the multistage gas-phase fragmentation behavior of phosphoserine- and phosphothreonine-containing peptides.

Literature DB >> 18181561

Mechanistic insights into the multistage gas-phase fragmentation behavior of phosphoserine- and phosphothreonine-containing peptides.

Amanda M Palumbo¹, Jetze J Tepe, Gavin E Reid.

Abstract

The increasing use of multistage tandem mass spectrometry (MS/MS and MS (3)) methods for comprehensive phosphoproteome analysis studies, as well as the emerging application of in silico spectral intensity prediction algorithms in enhanced database search analysis strategies, necessitate the development of an improved understanding of the mechanisms and other factors that affect the gas-phase fragmentation reactions of phosphorylated peptide ions. To address this need, we have examined the multistage collision-induced dissociation (CID) behavior of a set of singly and doubly charged phosphoserine- and phosphothreonine-containing peptide ions, as well as their regioselectively or uniformly deuterated derivatives, in a quadrupole ion trap mass spectrometer. Consistent with previous reports, the neutral loss of phosphoric acid (H 3PO 4) was observed as a dominant reaction pathway upon MS/MS. The magnitude of this loss was found to be highly dependent on the proton mobility of the precursor ion for both phosphoserine- and phosphothreonine-containing peptides. In contrast to that currently accepted in the literature, however, the results obtained in this study unequivocally demonstrate that the loss of H 3PO 4 does not predominantly occur via a "charge-remote" beta-elimination reaction. The observation of product ions corresponding to the loss of formaldehyde (CH 2O, 30 Da, or CD 2O, 32 Da) or acetaldehyde (CH 3CHO, 44 Da) upon MS (3) dissociation of the [M+ nH-H 3PO 4] ( n+ ) product ions from phosphoserine- and phosphothreonine-containing peptide ions, respectively, provide experimental evidence for a "charge-directed" mechanism involving an S N2 neighboring group participation reaction, resulting in the formation of a cyclic product ion. Potentially, these "diagnostic" MS (3) product ions may provide additional information to facilitate the characterization of phosphopeptides containing multiple potential phosphorylation sites.

Entities: Chemical

Mesh：

Substances：

Year: 2008 PMID： 18181561 DOI： 10.1021/pr0705136

Source DB: PubMed Journal: J Proteome Res ISSN： 1535-3893 Impact factor: 4.466

Keyword Cloud
Cited

31 in total

1. Defining intact protein primary structures from saliva: a step toward the human proteome project.

Authors: F Halgand; V Zabrouskov; S Bassilian; P Souda; J A Loo; K F Faull; D T Wong; J P Whitelegge
Journal: Anal Chem Date: 2012-05-02 Impact factor: 6.986

2. Akt-RSK-S6 kinase signaling networks activated by oncogenic receptor tyrosine kinases.

Authors: Albrecht Moritz; Yu Li; Ailan Guo; Judit Villén; Yi Wang; Joan MacNeill; Jon Kornhauser; Kam Sprott; Jing Zhou; Anthony Possemato; Jian Min Ren; Peter Hornbeck; Lewis C Cantley; Steven P Gygi; John Rush; Michael J Comb
Journal: Sci Signal Date: 2010-08-24 Impact factor: 8.192

3. Comparative assessment of site assignments in CID and electron transfer dissociation spectra of phosphopeptides discloses limited relocation of phosphate groups.

Authors: Nikolai Mischerikow; A F Maarten Altelaar; J Daniel Navarro; Shabaz Mohammed; Albert J R Heck
Journal: Mol Cell Proteomics Date: 2010-03-16 Impact factor: 5.911

4. Enhanced characterization of singly protonated phosphopeptide ions by femtosecond laser-induced ionization/dissociation tandem mass spectrometry (fs-LID-MS/MS).

Authors: Scott A Smith; Christine L Kalcic; Kyle A Safran; Paul M Stemmer; Marcos Dantus; Gavin E Reid
Journal: J Am Soc Mass Spectrom Date: 2010-10-01 Impact factor: 3.109

5. Unusual fragmentation of Pro-Ser/Thr-containing peptides detected in collision-induced dissociation spectra.

Authors: Katalin F Medzihradszky; Jonathan C Trinidad
Journal: J Am Soc Mass Spectrom Date: 2011-08-05 Impact factor: 3.109

6. Sulfonium ion derivatization, isobaric stable isotope labeling and data dependent CID- and ETD-MS/MS for enhanced phosphopeptide quantitation, identification and phosphorylation site characterization.

Authors: Yali Lu; Xiao Zhou; Paul M Stemmer; Gavin E Reid
Journal: J Am Soc Mass Spectrom Date: 2011-07-06 Impact factor: 3.109

Mechanistic insights into the multistage gas-phase fragmentation behavior of phosphoserine- and phosphothreonine-containing peptides.

1. Defining intact protein primary structures from saliva: a step toward the human proteome project.

2. Akt-RSK-S6 kinase signaling networks activated by oncogenic receptor tyrosine kinases.

3. Comparative assessment of site assignments in CID and electron transfer dissociation spectra of phosphopeptides discloses limited relocation of phosphate groups.

4. Enhanced characterization of singly protonated phosphopeptide ions by femtosecond laser-induced ionization/dissociation tandem mass spectrometry (fs-LID-MS/MS).

5. Unusual fragmentation of Pro-Ser/Thr-containing peptides detected in collision-induced dissociation spectra.

6. Sulfonium ion derivatization, isobaric stable isotope labeling and data dependent CID- and ETD-MS/MS for enhanced phosphopeptide quantitation, identification and phosphorylation site characterization.

7. Optimized Orbitrap HCD for quantitative analysis of phosphopeptides.

8. A new ion mobility-linear ion trap instrument for complex mixture analysis.

9. Comparison of MS(2)-only, MSA, and MS(2)/MS(3) methodologies for phosphopeptide identification.

10. Neighbor-directed histidine N (τ)-alkylation: A route to imidazolium-containing phosphopeptide macrocycles.