Quantitative trace analysis of a broad range of antiviral drugs in poultry muscle using column-switch liquid chromatography coupled to tandem mass spectrometry

Berendsen, B.J.A.; Wegh, Robin S.; Essers, M.L.; Stolker, A.A.M.; Weigel, Stefan

doi:10.1007/s00216-011-5581-3

Cited by 56 publications

(31 citation statements)

References 39 publications

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“…The situations where ∆pK a (the pK a difference between the base and acid) is larger than 3 almost exclusively result in salt formation, while situations with ∆pK a <0 almost exclusively result in cocrystal formation, but 0<∆pK a <3 can lead to either salts or co-crystals, or even complexes with partial proton transfer, with the location of the acidic proton dependent on the specific crystal packing environment [17]. Table 1 presents the ΔpK a values calculated from the pK a values of umifenovir and dicarboxylic acids given in the literature [18]. …”

Section: Resultsmentioning

confidence: 99%

Characterization and Physicochemical Evaluation of Molecular Complexes Formed Between Umifenovir and Dicarboxylic Acids

Kons¹,

Be̅rziņš²,

Krūkle-Bērziņa³

et al. 2014

Latvian Journal of Chemistry

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The paper reports the investigation of three umifenovir molecular complexes with dicarboxylic acids, prepared to improve the bioavailability of this drug. All three molecular complexes were investigated by powder X-ray diffraction, infrared spectroscopy, and solid-state nuclear magnetic resonance spectroscopy. The solubility and thermal properties were determined as well. Polymorph and solvate screening of umifenovir molecular complexes were performed by recrystallization from various solvents, as well as neat and solvent-drop grinding.

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Section: Resultsmentioning

confidence: 99%

Characterization and Physicochemical Evaluation of Molecular Complexes Formed Between Umifenovir and Dicarboxylic Acids

Kons¹,

Be̅rziņš²,

Krūkle-Bērziņa³

et al. 2014

Latvian Journal of Chemistry

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“…Arbidol is a relatively strong base with the pKa value equaling 6.0 (for the dimethylamino group) [27]. It is widely accepted in the literature that whether an API and a guest molecule form a salt or cocrystal can be predicted in terms of the ∆pKa rule (ΔpKa = pKa (base) − pKa (acid) ) [28][29][30].…”

Section: Crystal Structuresmentioning

confidence: 99%

“…As it has been mentioned, Arb is a relatively strong base with pKa value near 6.0 [27]. Therefore, the solubility of the drug, as well as its salts, in aqueous solutions is expected to be pH-dependent.…”

Section: Aqueous Dissolution Studymentioning

confidence: 99%

Crystal Structures, Thermal Analysis, and Dissolution Behavior of New Solid Forms of the Antiviral Drug Arbidol with Dicarboxylic Acids

et al. 2015

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Salts of the antiviral drug arbidol (umifenovir) (Arb) with maleate (Mlc) and fumarate (Fum) anions have been obtained, and their crystal structures have been described. The crystal structure of arbidol maleate has been redetermined by single crystal X-ray diffraction at 180K. A new arbidol cocrystal in zwitterion form with succinic acid (Suc) has also been found and characterized. The arbidol zwitterion was not previously seen in any of the drug crystal forms, and the [Arb + Suc] cocrystal seems to be the first found instance. Analysis of the conformational preferences of the arbidol molecule in the crystal structures has shown that it adopts two types of conformations, namely "open" and "closed" ones. Thermal stability of the arbidol salts and cocrystal have been analyzed by means of differential scanning calorimetry, thermogravimetric, and mass-spectrometry analysis. The dissolution study of the arbidol salts and cocrystal performed in aqueous buffer solutions with pH 1.2 and 6.8 has shown that both the salts and the cocrystal dissolve incongruently to form an arbidol hydrochloride monohydrate at pH 1.2 and an OPEN ACCESSCrystals 2015, 5 651 arbidol base at pH 6.8, respectively. The cocrystal reaches the highest solubility level in both pH 1.2 and pH 6.8 solutions.

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“…(WHO, 2005). Analytical methods have been developed to test for residues of some antiviral drugs in poultry meat (Berendsen et al, 2012), but widespread adoption of antiviral drugs by livestock industries has thus far been averted. Residues of antiviral drugs do not currently form a part of routine residues testing plans in Europe.…”

Section: (V) Antiviral Drugsmentioning

confidence: 99%

Potential impacts of climate change on veterinary medicinal residues in livestock produce: An island of Ireland perspective††This paper is one of a series of reviews on “Climate Change and Food Safety – an Island of Ireland perspective”.

Cooper

McMahon

Fairweather

et al. 2015

Trends in Food Science & Technology

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Quantitative trace analysis of a broad range of antiviral drugs in poultry muscle using column-switch liquid chromatography coupled to tandem mass spectrometry

Cited by 56 publications

References 39 publications

Characterization and Physicochemical Evaluation of Molecular Complexes Formed Between Umifenovir and Dicarboxylic Acids

Characterization and Physicochemical Evaluation of Molecular Complexes Formed Between Umifenovir and Dicarboxylic Acids

Crystal Structures, Thermal Analysis, and Dissolution Behavior of New Solid Forms of the Antiviral Drug Arbidol with Dicarboxylic Acids

Potential impacts of climate change on veterinary medicinal residues in livestock produce: An island of Ireland perspective††This paper is one of a series of reviews on “Climate Change and Food Safety – an Island of Ireland perspective”.

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