Comparison of the activation time effects and the internal energy distributions for the CID, PQD and HCD excitation modes

Farid Ichou; Adrian Schwarzenberg; Denis Lesage; Sandra Alves; Christophe Junot; Xavier Machuron-Mandard; Jean-Claude Tabet

doi:10.1002/jms.3365

Comparison of the activation time effects and the internal energy distributions for the CID, PQD and HCD excitation modes

J Mass Spectrom. 2014 Jun;49(6):498-508. doi: 10.1002/jms.3365.

Authors

Farid Ichou¹, Adrian Schwarzenberg, Denis Lesage, Sandra Alves, Christophe Junot, Xavier Machuron-Mandard, Jean-Claude Tabet

Affiliation

¹ Institut Parisien de Chimie Moléculaire, UMR 8232, UPMC, Paris CEDEX 05, 75252, France.

PMID: 24913402
DOI: 10.1002/jms.3365

Abstract

Reproducibility among different types of excitation modes is a major bottleneck in the field of tandem mass spectrometry library development in metabolomics. In this study, we specifically evaluated the influence of collision voltage and activation time parameters on tandem mass spectrometry spectra for various excitation modes [collision-induced dissociation (CID), pulsed Q dissociation (PQD) and higher-energy collision dissociation (HCD)] of Orbitrap-based instruments. For this purpose, internal energy deposition was probed using an approach based on Rice-Rampserger-Kassel-Marcus modeling with three thermometer compounds of different degree of freedom (69, 228 and 420) and a thermal model. This model treats consecutively the activation and decomposition steps, and the survival precursor ion populations are characterized by truncated Maxwell-Boltzmann internal energy distributions. This study demonstrates that the activation time has a significant impact on MS/MS spectra using the CID and PQD modes. The proposed model seems suitable to describe the multiple collision regime in the PQD and HCD modes. Linear relationships between mean internal energy and collision voltage are shown for the latter modes and the three thermometer molecules. These results suggest that a calibration based on the collision voltage should provide reproducible for PQD, HCD to be compared with CID in tandem in space instruments. However, an important signal loss is observed in PQD excitation mode whatever the mass of the studied compounds, which may affect not only parent ions but also fragment ions depending on the fragmentation parameters. A calibration approach for the CID mode based on the variation of activation time parameter is more appropriate than one based on collision voltage. In fact, the activation time parameter in CID induces a modification of the collisional regime and thus helps control the orientation of the fragmentation pathways (competitive or consecutive dissociations).

Keywords: CID; HCD; PQD; RRKM modeling; activation time; internal energy distribution; metabolomics.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Enkephalin, Leucine
Ions / chemistry*
Models, Chemical*
Reproducibility of Results
Tandem Mass Spectrometry / methods*

Substances

Ions
Enkephalin, Leucine