Controlling the diversity of ion-induced fragmentation pathways by -methylation of amino acids
We present a combined experimental and theoretical study of the fragmentation of singly and doubly N -methylated glycine (sarcosine and N , N -dimethyl glycine, respectively) induced by low-energy (keV) O 6+ ions. Multicoincidence mass spectrometry techniques and quantum chemistry simulations ( ab i...
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Published in | Physical chemistry chemical physics : PCCP Vol. 24; no. 2; pp. 941 - 954 |
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Main Authors | , , , , , , , , , , |
Format | Journal Article |
Published |
04.01.2022
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Online Access | Get full text |
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Summary: | We present a combined experimental and theoretical study of the fragmentation of singly and doubly
N
-methylated glycine (sarcosine and
N
,
N
-dimethyl glycine, respectively) induced by low-energy (keV) O
6+
ions. Multicoincidence mass spectrometry techniques and quantum chemistry simulations (
ab initio
molecular dynamics and density functional theory) allow us to characterise different fragmentation pathways as well as the associated mechanisms. We focus on the fragmentation of doubly ionised species, for which coincidence measurements provide unambiguous information on the origin of the various charged fragments. We have found that single
N
-methylation leads to a larger variety of fragmentation channels than in no methylation of glycine, while double
N
-methylation effectively closes many of these fragmentation channels, including some of those appearing in pristine glycine. Importantly, the closure of fragmentation channels in the latter case does not imply a protective effect by the methyl group.
In a joint experimental and theoretical study, we report on the fragmentation of singly and doubly
N
-methylated glycine induced by low-energy (keV) O
6+
ions. |
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Bibliography: | dimethylglycine. See DOI 10.1039/d1cp04097a Electronic supplementary information (ESI) available: Geometries of the neutral conformers and statistics of the molecular dynamics for methylglycine and , N |
ISSN: | 1463-9076 1463-9084 |
DOI: | 10.1039/d1cp04097a |