Electron ionization mass spectra of novel 2,3:4,5‐bis‐<i>O</i>‐(1‐methylethylidene)‐β‐<scp>D</scp>‐fructopyranose derivatives and related sugar sulfamates

Caldwell, Gary W.; Sorgi, Kirk L.; Scott, L. Keith; Maryanoff, Bruce E.; Maryanoff, Cynthia A.; Masucci, John A.; Nortey, Samuel; Sisco, W.R.; Micheel, Arthur P; Ko, Chan-Yan

doi:10.1002/oms.1210241204

Cited by 6 publications

(4 citation statements)

References 9 publications

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“…The MS (NH 3-CI) analysis of unchanged TPM revealed a significant protonated ammonium cation [M+ NH 4 "lat mlz 357. Based on previous electron ionization MS studies of TPM [16], a fragmentation scheme illustrating these neutral loss products is shown in Figure 2. The MS (NH 3-CI) spectra contained many characteristic fragment cations based on neutral loss of acetone from the dioxolane rings (m/z 299, and 241), neutral loss of HOS0 2NH2 (m/z 243) and a combination of both (m/z 185, 127, 113).…”

Section: As Shown Inmentioning

confidence: 99%

Metabolism and excretion of the antiepileptic/antimigraine drug, topiramate in animals and humans

Caldwell

Masucci

et al. 2005

European Journal of Drug Metabolism and Pharmacokinetics

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The metabolism and excretion of 2,3:4,5-bis-O-(1-methylethylidene)-beta-D-fructopyranose sulfamate (TOPAMAX, topiramate, TPM) have been investigated in animals and humans. Radiolabeled [14C] TPM was orally administered to mice, rats, rabbits, dogs and humans. Plasma, urine and fecal samples were collected and analyzed. TPM and a total of 12 metabolites were isolated and identified in these samples. Metabolites were formed by hydroxylation at the 7- or 8-methyl of an isopropylidene of TPM followed by rearrangement, hydroxylation at the 10-methyl of the other isopropylidene, hydrolysis at the 2,3-O-isopropylidene, hydrolysis at the 4,5-O-isopropylidene, cleavage at the sulfamate group, glucuronide conjugation and sulfate conjugation. A large percentage of unchanged TPM was recovered in animal and human urine. The most dominant metabolite of TPM in mice, male rats, rabbits and dogs appeared to be formed by the hydrolysis of the 2,3-O-isopropylidene group.

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Section: As Shown Inmentioning

confidence: 99%

Metabolism and excretion of the antiepileptic/antimigraine drug, topiramate in animals and humans

Caldwell

Masucci

et al. 2005

European Journal of Drug Metabolism and Pharmacokinetics

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“…As observed for other carbohydrate derivatives containing the 1,2-0-isopropylidene group, [14][15][16][17] fragmentation in this unit results in the elimination of acetone leading to the base peak at m/z 253, which appears to be most prevalent for compound 1.…”

Section: Metastable Ion and High-energy Cid Spectra Ofmentioning

confidence: 55%

Characterization of stereoisomeric furanosidic derivatives by direct chemical ionization mass spectrometry and liquid secondary ion mass spectrometry with tandem mass spectrometry. (Part II)

Borges

Ferreira

Heuvel

et al. 1997

Rapid Commun. Mass Spectrom.

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The present study deals with the mass spectrometric characterization of furanosidic compounds containing a 1,2-O-isopropylidene group using different mass spectrometric techniques: chemical ionization mass spectrometry and liquid secondary ion mass spectrometry together with metastable ion analysis and collision-induced dissociation. Common fragmentation differences relate to the extent of the loss of water and the elimination of acetone. It is also shown that the introduction of a stable charge centre (Li + ) in the molecules is critical for observing a rearrangement involving hydrogen transfer in one of the two stereoisomeric pairs examined.

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“…Further work using IR, Raman, and 13 C NMR on the 2:1 bis(betaine) sulfamate (see section ) has been reported . An EI/MS study of seven bis- O -(1-methylethylene)fructopyranose sulfamates including the well-known anticonvulsant topiramate 10 have revealed the fragmentation patterns, and the mechanisms involved are discussed …”

Section: Sulfamic Acidmentioning

confidence: 97%

“…55 An EI/MS study of seven bis-O-(1-methylethylene)fructopyranose sulfamates including the well-known anticonvulsant topiramate 10 have revealed the fragmentation patterns, and the mechanisms involved are discussed. 56…”

Section: Magnetic and Spectroscopic Studiesmentioning

confidence: 99%

Sulfamic Acid and Its N- and O-Substituted Derivatives

2013

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Electron ionization mass spectra of novel 2,3:4,5‐bis‐O‐(1‐methylethylidene)‐β‐D‐fructopyranose derivatives and related sugar sulfamates

Cited by 6 publications

References 9 publications

Metabolism and excretion of the antiepileptic/antimigraine drug, topiramate in animals and humans

Metabolism and excretion of the antiepileptic/antimigraine drug, topiramate in animals and humans

Characterization of stereoisomeric furanosidic derivatives by direct chemical ionization mass spectrometry and liquid secondary ion mass spectrometry with tandem mass spectrometry. (Part II)

Sulfamic Acid and Its N- and O-Substituted Derivatives

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