N-Protonated Isomers and Coulombic Barriers to Dissociation of Doubly Protonated Ala{sub 8}Arg
Collision-induced dissociation (or tandem mass spectrometry, MS/MS) of a protonated peptide results in a spectrum of fragment ions that is useful for inferring amino acid sequence. This is now commonplace and a foundation of proteomics. The underlying chemical and physical processes are believed to...
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| Veröffentlicht in: | Journal of the American Society for Mass Spectrometry 2017-10, Vol.28 (10) |
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| creator | Haeffner, Fredrik Irikura, Karl K. |
| description | Collision-induced dissociation (or tandem mass spectrometry, MS/MS) of a protonated peptide results in a spectrum of fragment ions that is useful for inferring amino acid sequence. This is now commonplace and a foundation of proteomics. The underlying chemical and physical processes are believed to be those familiar from physical organic chemistry and chemical kinetics. However, first-principles predictions remain intractable because of the conflicting necessities for high accuracy (to achieve qualitatively correct kinetics) and computational speed (to compensate for the high cost of reliable calculations on such large molecules). To make progress, shortcuts are needed. Inspired by the popular mobile proton model, we have previously proposed a simplified theoretical model in which the gas-phase fragmentation pattern of protonated peptides reflects the relative stabilities of N-protonated isomers, thus avoiding the need for transition-state information. For singly protonated Ala{sub n} (n = 3–11), the resulting predictions were in qualitative agreement with the results from low-energy MS/MS experiments. Here, the comparison is extended to a model tryptic peptide, doubly protonated Ala{sub 8}Arg. This is of interest because doubly protonated tryptic peptides are the most important in proteomics. In comparison with experimental results, our model seriously overpredicts the degree of backbone fragmentation at N{sub 9}. We offer an improved model that corrects this deficiency. The principal change is to include Coulombic barriers, which hinder the separation of the product cations from each other. Coulombic barriers may be equally important in MS/MS of all multiply charged peptide ions. . |
| doi_str_mv | 10.1007/S13361-017-1719-7 |
| format | Article |
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This is now commonplace and a foundation of proteomics. The underlying chemical and physical processes are believed to be those familiar from physical organic chemistry and chemical kinetics. However, first-principles predictions remain intractable because of the conflicting necessities for high accuracy (to achieve qualitatively correct kinetics) and computational speed (to compensate for the high cost of reliable calculations on such large molecules). To make progress, shortcuts are needed. Inspired by the popular mobile proton model, we have previously proposed a simplified theoretical model in which the gas-phase fragmentation pattern of protonated peptides reflects the relative stabilities of N-protonated isomers, thus avoiding the need for transition-state information. For singly protonated Ala{sub n} (n = 3–11), the resulting predictions were in qualitative agreement with the results from low-energy MS/MS experiments. Here, the comparison is extended to a model tryptic peptide, doubly protonated Ala{sub 8}Arg. This is of interest because doubly protonated tryptic peptides are the most important in proteomics. In comparison with experimental results, our model seriously overpredicts the degree of backbone fragmentation at N{sub 9}. We offer an improved model that corrects this deficiency. The principal change is to include Coulombic barriers, which hinder the separation of the product cations from each other. 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This is now commonplace and a foundation of proteomics. The underlying chemical and physical processes are believed to be those familiar from physical organic chemistry and chemical kinetics. However, first-principles predictions remain intractable because of the conflicting necessities for high accuracy (to achieve qualitatively correct kinetics) and computational speed (to compensate for the high cost of reliable calculations on such large molecules). To make progress, shortcuts are needed. Inspired by the popular mobile proton model, we have previously proposed a simplified theoretical model in which the gas-phase fragmentation pattern of protonated peptides reflects the relative stabilities of N-protonated isomers, thus avoiding the need for transition-state information. For singly protonated Ala{sub n} (n = 3–11), the resulting predictions were in qualitative agreement with the results from low-energy MS/MS experiments. Here, the comparison is extended to a model tryptic peptide, doubly protonated Ala{sub 8}Arg. This is of interest because doubly protonated tryptic peptides are the most important in proteomics. In comparison with experimental results, our model seriously overpredicts the degree of backbone fragmentation at N{sub 9}. We offer an improved model that corrects this deficiency. The principal change is to include Coulombic barriers, which hinder the separation of the product cations from each other. Coulombic barriers may be equally important in MS/MS of all multiply charged peptide ions. .</description><subject>AFFINITY</subject><subject>COLLISIONS</subject><subject>COMPARATIVE EVALUATIONS</subject><subject>DIFFUSION BARRIERS</subject><subject>DISSOCIATION</subject><subject>FORECASTING</subject><subject>FRAGMENTATION</subject><subject>INFORMATION</subject><subject>INSTRUMENTATION RELATED TO NUCLEAR SCIENCE AND TECHNOLOGY</subject><subject>ISOMERS</subject><subject>MASS SPECTROSCOPY</subject><subject>MOLECULES</subject><subject>PEPTIDES</subject><subject>PROTONS</subject><subject>SPECTRA</subject><issn>1044-0305</issn><issn>1879-1123</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2017</creationdate><recordtype>article</recordtype><recordid>eNpNz01LAzEQBuAgCtbqD_AW8BzNZOpO9lhbv6CooF4t-djVyHYHNulBxP_uih48zcvLywMjxDHoU9Cazh4BsQKlgRQQ1Ip2xAQs1QrA4O6Y9WymNOrzfXGQ87seh7qmiXi5Uw8DF-5daaK8zbxphixdH-WCtx1vfArywg1D-qkLy2XKmUNyJXEvuZVL3vruQ_4z5p37zFsv7dd8eD0Ue63rcnP0d6fi-eryaXGjVvfXt4v5SjEAFjWrvSVjiSof2woJtCXbWm-09tY36DEahKqyrkVqY0RTeRMRyLnxp0A4FSe_LueS1jmk0oS3wH3fhLI2ZoRHHL8Bp95Vuw</recordid><startdate>20171015</startdate><enddate>20171015</enddate><creator>Haeffner, Fredrik</creator><creator>Irikura, Karl K.</creator><scope>OTOTI</scope></search><sort><creationdate>20171015</creationdate><title>N-Protonated Isomers and Coulombic Barriers to Dissociation of Doubly Protonated Ala{sub 8}Arg</title><author>Haeffner, Fredrik ; Irikura, Karl K.</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-o113t-49b8728776bdf63710878f8b200b8be3b3d231668af37fdd326b2d317aa030c73</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2017</creationdate><topic>AFFINITY</topic><topic>COLLISIONS</topic><topic>COMPARATIVE EVALUATIONS</topic><topic>DIFFUSION BARRIERS</topic><topic>DISSOCIATION</topic><topic>FORECASTING</topic><topic>FRAGMENTATION</topic><topic>INFORMATION</topic><topic>INSTRUMENTATION RELATED TO NUCLEAR SCIENCE AND TECHNOLOGY</topic><topic>ISOMERS</topic><topic>MASS SPECTROSCOPY</topic><topic>MOLECULES</topic><topic>PEPTIDES</topic><topic>PROTONS</topic><topic>SPECTRA</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Haeffner, Fredrik</creatorcontrib><creatorcontrib>Irikura, Karl K.</creatorcontrib><collection>OSTI.GOV</collection><jtitle>Journal of the American Society for Mass Spectrometry</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Haeffner, Fredrik</au><au>Irikura, Karl K.</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>N-Protonated Isomers and Coulombic Barriers to Dissociation of Doubly Protonated Ala{sub 8}Arg</atitle><jtitle>Journal of the American Society for Mass Spectrometry</jtitle><date>2017-10-15</date><risdate>2017</risdate><volume>28</volume><issue>10</issue><issn>1044-0305</issn><eissn>1879-1123</eissn><abstract>Collision-induced dissociation (or tandem mass spectrometry, MS/MS) of a protonated peptide results in a spectrum of fragment ions that is useful for inferring amino acid sequence. This is now commonplace and a foundation of proteomics. The underlying chemical and physical processes are believed to be those familiar from physical organic chemistry and chemical kinetics. However, first-principles predictions remain intractable because of the conflicting necessities for high accuracy (to achieve qualitatively correct kinetics) and computational speed (to compensate for the high cost of reliable calculations on such large molecules). To make progress, shortcuts are needed. Inspired by the popular mobile proton model, we have previously proposed a simplified theoretical model in which the gas-phase fragmentation pattern of protonated peptides reflects the relative stabilities of N-protonated isomers, thus avoiding the need for transition-state information. For singly protonated Ala{sub n} (n = 3–11), the resulting predictions were in qualitative agreement with the results from low-energy MS/MS experiments. Here, the comparison is extended to a model tryptic peptide, doubly protonated Ala{sub 8}Arg. This is of interest because doubly protonated tryptic peptides are the most important in proteomics. In comparison with experimental results, our model seriously overpredicts the degree of backbone fragmentation at N{sub 9}. We offer an improved model that corrects this deficiency. The principal change is to include Coulombic barriers, which hinder the separation of the product cations from each other. Coulombic barriers may be equally important in MS/MS of all multiply charged peptide ions. .</abstract><cop>United States</cop><doi>10.1007/S13361-017-1719-7</doi></addata></record> |
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| subjects | AFFINITY COLLISIONS COMPARATIVE EVALUATIONS DIFFUSION BARRIERS DISSOCIATION FORECASTING FRAGMENTATION INFORMATION INSTRUMENTATION RELATED TO NUCLEAR SCIENCE AND TECHNOLOGY ISOMERS MASS SPECTROSCOPY MOLECULES PEPTIDES PROTONS SPECTRA |
| title | N-Protonated Isomers and Coulombic Barriers to Dissociation of Doubly Protonated Ala{sub 8}Arg |
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