Gram-negative bacterial lipid A analysis by negative electrospray ion trap mass spectrometry: Stepwise dissociations of deprotonated species under low energy CID conditions

Madalinski, Geoffrey; Fournier, Françoise; Wind, Franck-Lionel; Afonso, Carlos; Tabet, Jean‐Claude

doi:10.1016/j.ijms.2005.12.049

Cited by 31 publications

(64 citation statements)

References 32 publications

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“…4B ). The frequency of the loss of phosphoric acid from the position O-1 was signifi cantly higher than from O-4' during ESI-MS 2 analysis due to the lability of glycosidically linked P group ( 28,31 ). Interpretation of the observed fragment ions is presented in Fig.…”

Section: Esi-ms Analysis Of Partially Deo-acylated Lipid Amentioning

confidence: 99%

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Structural analysis of the lipid A isolated from Hafnia alvei 32 and PCM 1192 lipopolysaccharides

Łukasiewicz

Jachymek

Niedziela

et al. 2010

Journal of Lipid Research

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Section: Esi-ms Analysis Of Partially Deo-acylated Lipid Amentioning

confidence: 99%

“…I). Because the obtained data suggested the E. coli -type structure of studied lipid A, ESI-MS n spectra were compared with data published previously for lipid A of E. coli (29)(30)(31).…”

Section: Esi-ms/msmentioning

confidence: 99%

Structural analysis of the lipid A isolated from Hafnia alvei 32 and PCM 1192 lipopolysaccharides

Łukasiewicz

Jachymek

Niedziela

et al. 2010

Journal of Lipid Research

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“…As shown previously, UVPD results in structure-specific glycosidic and cross-ring fragments of lipid A and affords richer fragmentation patterns when compared to conventional collisional activation methods [27–35]. Multi-stage MS n strategies have also been important for structural characterization of lipid A [36–38]. Recent work by the Goodlett group successfully determined the structures of various lipid A using an automated hierarchical tandem MS algorithm known as HitMS [37, 38].…”

Section: Introductionmentioning

confidence: 99%

Characterization of Lipid A Variants by Energy-Resolved Mass Spectrometry: Impact of Acyl Chains

Crittenden

Akin

Morrison

et al. 2016

J. Am. Soc. Mass Spectrom.

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Lipid A molecules consist of a diglucosamine sugar core with a number of appended acyl chains which vary in their length and connectivity. Because of the challenging nature of characterizing these molecules and differentiating between isomeric species, an energy-resolved MS/MS strategy was undertaken to track the fragmentation trends and map genealogies of product ions originating from consecutive cleavages of acyl chains. Generalizations were developed based on the number and locations of the primary and secondary acyl chains as well as variations in preferential cleavages arising from the location of the phosphate groups. Secondary acyl chain cleavage occurs most readily for lipid A species at the 3′ position, followed by primary acyl chain fragmentation at both the 3′ and 3 positions. In the instances of bisphosphorylated lipid A variants, phosphate loss occurs readily in conjunction with the most favorable primary and secondary acyl chain cleavages.

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“…Three competing fragmentation pathways are thus proposed for MccC7-C51*: MccC7-C51 and MccC7-C51* show that, for such even-electron complex systems, the isomerization into ion-dipole complexes takes place before dissociation. This behavior is well known for a large class of chemical compounds including organic and biological molecules, such as certain amino steroids [12], glycoconjugates [14], steroid fatty acids [26], DNA adduct steroids [13], lipopolysaccharides [27], and peptides [28]. If the complex life time is sufficiently large, due to the relative low internal energy compared to the dissociation energy threshold, internal proton transfer can occur, resulting from the formation of complementary ion pairs.…”

Section: Positive Ions Generated From Mccc7-c51 Mccc7-c51* and Pepcmentioning

confidence: 97%

Collision induced dissociation-based characterization of nucleotide peptides: Fragmentation patterns of microcin C7–C51, an antimicrobial peptide produced by Escherichia coli

Petit

Zirah

Rebuffat

et al. 2008

J. Am. Soc. Mass Spectrom.

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Covalent© protein-nucleic© acid© conjugates© form© an© original© class© of© compounds© that© occur© in nature© or© can© be© generated© in© vitro© through© cross-linking© to© investigate© domains© involved© in protein/nucleic© acid© interactions.© Their© mass© spectrometry© fragmentation© patterns© are© poorly characterized.© We© have© used© electrospray-ionization© mass© spectrometry© (ESI-MS)© combined with© collision-induced© dissociation© (CID)© to© characterize© microcin© C7-C51,© an© antimicrobial nucleotide© peptide© that© targets© aspartyl-tRNA© synthetase© and© inhibits© translation.© The© fragments© of© microcin© C7-C51© were© analyzed© in© positive-© and© negative-ion© modes© and© compared with©those©of©the©corresponding©unmodified©heptapeptide©and©to©the©derived©aspartyl-adenylate.©The©positive-©and©negative-ion©mode©fragments©of©microcin©C7-C51©provided information©on©both©the©nucleotide©and©peptide©moieties.©Accurate©mass©measurement obtained© using© an© LTQ© Orbitrap© instrument© was© a© key© factor© for© a© comprehensive© interpretation© of© the© fragments.© The© experimental© results© obtained© permitted© the© proposal© of© stepwise fragmentation© pathways© involving© ion-© dipole© complexes.© The© data© provide© a© better© understanding© of© nucleotide© peptide© fragmentation© in© the© gas© phase

show abstract

Gram-negative bacterial lipid A analysis by negative electrospray ion trap mass spectrometry: Stepwise dissociations of deprotonated species under low energy CID conditions

Cited by 31 publications

References 32 publications

Structural analysis of the lipid A isolated from Hafnia alvei 32 and PCM 1192 lipopolysaccharides

Structural analysis of the lipid A isolated from Hafnia alvei 32 and PCM 1192 lipopolysaccharides

Characterization of Lipid A Variants by Energy-Resolved Mass Spectrometry: Impact of Acyl Chains

Collision induced dissociation-based characterization of nucleotide peptides: Fragmentation patterns of microcin C7–C51, an antimicrobial peptide produced by Escherichia coli

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