Electrochemical reduction of ketoprofen and its determination in pharmaceutical dosage forms by differential-pulse polarography

Amankwa, Lawrence N.; Chatten, L.G.

doi:10.1039/an9840900057

Cited by 16 publications

(8 citation statements)

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“…6). The values found for KP were in good agreement with that previously reported by Amankwa and Chatten (29) in the same conditions. For BP, these values are in the same range as the values found by Nadjo and Savéant (30) in previous experiments performed in acetonitrile solutions in the cavity of an EPR spectrometer.…”

Section: Electrochemical Determinationssupporting

confidence: 92%

Comparison of DNA Damage Photoinduced by Ketoprofen, Fenofibric Acid and Benzophenone via Electron and Energy Transfer¶

Lhiaubet

Paillous

Chouini–Lalanne

2007

Photochemistry and Photobiology

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Ketoprofen (KP) and fenofibrate, respectively, anti-inflammatory and hypolipidemiant agents, promote anormal photosensitivity in patients and may induce photoallergic cross-reactions correlated to their benzophenone-like structure. Here, their ability to photosensitize the degradation of biological targets was particularly investigated in DNA. The photosensitization of DNA damage by KP and fenofibric acid (FB), the main metabolite of fenofibrate, and their parent compound, benzophenone (BZ), was examined on a 32 P-end-labeled synthetic oligonucleotide in phosphatebuffered solution using gel sequencing experiments. Upon irradiation at Ͼ 320 nm, piperidine-sensitive lesions were induced in single-stranded oligonucleotides by KP, FB and BZ at all G sites to the same extent. This pattern of damage, enhanced in D 2 O is characteristic of a Type-II mechanism. Spin trapping experiments using 2,2,6,6-tetramethyl-4-piperidone have confirmed the production of singlet oxygen during drug photolysis. On double-stranded oligonucleotides, highly specific DNA break occurred selectively at 5-G of a 5-GG-3 sequence, after alkali treatment. Prolonged irradiation led to the degradation of all G residues, with efficiency decreasing in the order 5-GG Ͼ 5-GA Ͼ 5-GC Ͼ 5-GT, in good agreement with the calculated lowest ionization potentials of stacked nucleobase models supporting the assumption of a Type-I mechanism involving electron transfer, also observed to a lesser extent with adenine. Cytosine sites were also affected but the action of mannitol which selectively inhibited cytosine lesions suggests, in this case, the involvement of hydroxyl radical, also detected by electronic paramagnetic resonance using 5,5-dimethyl-1pyrrolidine-1-oxide as spin trap. On a double-stranded 32 P-end-labeled 25-mer oligonucleotide containing TT and TTT sequences, the three compounds were found to photosensitize by triplet-triplet energy transfer the ¶Posted on the website on formation of cyclobutane thymine dimers detected using T4 endonuclease V.

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Section: Electrochemical Determinationssupporting

confidence: 92%

Comparison of DNA Damage Photoinduced by Ketoprofen, Fenofibric Acid and Benzophenone via Electron and Energy Transfer¶

Lhiaubet

Paillous

Chouini–Lalanne

2007

Photochemistry and Photobiology

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“…Analogously to those aromatic ketone derivatives reported in [16][17][18][19][20][21], a single reduction peak of trepibutone at about À1.1 V in a two-electron, two-proton addition was observed in aqueous solution, and two separate peaks were seen in organic medium from two successive one-electron transfers, demonstrating that the free radical occurred [23][24][25]. Obviously, the voltammetric behavior of trepibutone at a PGE was different from that at a mercury electrode, although an aqueous solution was still used as the experimental medium in this work.…”

Section: Voltammetric Behavior Of Trepibutonementioning

confidence: 97%

“…The polarographic behavior of fenofibrate, ketoprofen, amiodarone, mebendazole and flubendazole, all aromatic ketone derivatives, have been studied in aqueous and organic media by Yardimci and Ö zaltin [16], Li et al [17], Amankwa and Chatten [18], Tan et al [19], Pinilla and Hemadez [20] and El-Enamy et al [21], respectively. The results demonstrated that the carbonyl moiety in the benzoyl group in these compounds was electroactive.…”

Section: Voltammetric Behavior Of Trepibutonementioning

confidence: 99%

Voltammetric behavior and square-wave voltammetric determination of trepibutone at a pencil graphite electrode

Gao

Song

2005

Journal of Electroanalytical Chemistry

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“…In view of its chemical structure, amiodarone was known as (2-butyl-3-benzofuranyl)[4-[2-(diethylamino)ethoxy]-3,5-diiodophenyl]methanone hydrochloride, and belongs to benzoyl derivatives. The polarographic behaviors of benzoyl derivatives such as fenofibrate, ketoprofen, amiodarone, mebendazole and flubendazole have been studied in aqueous and organic media and used for analytical purpose, [22][23][24][25][26] respectively. All these derivatives showed a polarographic reduction wave, which was attributed to the reduction of the electroactive benzoyl group via a two-electron and two-proton addition.…”

Section: Voltammetric Behavior Of Amiodaronementioning

confidence: 99%

Catalytic Adsorptive Stripping Voltammetry at a Carbon Paste Electrode for the Determination of Amiodarone

2006

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Voltammetry using solid electrodes usually suffers from the contamination due to the deposition of the redox products of analytes on the electrode surface. The contamination has resulted in poor reproducibility and overelaborate operation procedures. The use of the chemical catalysis of oxidant on the reduction product of analyte not only can eliminate the contamination of analyte to solid electrodes but also can improve the faradaic response of analyte. This work introduced both the catalysis of oxidant K 2 S 2 O 8 and the enhancement of surfactant Triton X-100 on the faraday response of amiodarone into an adsorptive stripping voltammetry at a carbon paste electrode for the determination of amiodarone. The method exhibits high sensitivity, good reproducibility and simple operation procedure. In 0.2 mol•L -1 HOAc-NaOAc buffer (pH＝5.3) containing 2.2×10 -2 mol•L -1 K 2 S 2 O 8 and 0.002% Triton X-100, the 2.5th-order derivative stripping peak current of the catalytic wave at 0.3 V (vs. Ag/AgCl) is rectilinear to amiodarone concentration in the range of 2.0×10 -10 -2.3×10 -8 mol•L -1 with a detection limit of 1.5×10-10 mol•L -1 after accumulation at 0 V for 30 s.

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Electrochemical reduction of ketoprofen and its determination in pharmaceutical dosage forms by differential-pulse polarography

Cited by 16 publications

References 0 publications

Comparison of DNA Damage Photoinduced by Ketoprofen, Fenofibric Acid and Benzophenone via Electron and Energy Transfer¶

Comparison of DNA Damage Photoinduced by Ketoprofen, Fenofibric Acid and Benzophenone via Electron and Energy Transfer¶

Voltammetric behavior and square-wave voltammetric determination of trepibutone at a pencil graphite electrode

Catalytic Adsorptive Stripping Voltammetry at a Carbon Paste Electrode for the Determination of Amiodarone

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