Oxidative transformation of ciprofloxacin by alkaline permanganate – A kinetic and mechanistic study

This spectroscopic study presents the kinetics and degradation pathways of oxidation of ciprofloxacin by permanganate in alkaline medium at constant ionic strength of 0.04 mol⁻³. Orders with respect to substrate, oxidant and alkali concentrations were determined. Effect of ionic strength and solvent polarity of the medium on the rate of the reaction was studied. The oxidation products were identified by LC-ESI-MS technique. Product characterization of ciprofloxacin reaction mixtures indicates the formation of three major products corresponding to m/z 263, 306, and 348 (corresponding to full or partial dealkylation of the piperazine ring). The piperazine moiety of ciprofloxacin is the predominant oxidative site to KMnO₄. Product analyses showed that oxidation by permanganate results in dealkylation at the piperazine moiety of ciprofloxacin, with the quinolone ring essentially intact. The reaction kinetics and product characterization point to a reaction mechanism that likely begins with formation of a complex between ciprofloxacin and the KMnO₄, followed by oxidation at the aromatic N1 atom of piperazine moiety to generate an anilinyl radical intermediate. The radical intermediates subsequently undergo N-dealkylation. Investigations of the reaction at different temperatures allowed the determination of the activation parameters with respect to the slow step of proposed mechanism. The proposed mechanism and the derived rate laws are consistent with the observed kinetics.     

Osmium(VIII) mediated oxidation of mercury(I) by cerium(IV) in aqueous sulphuric acid – a kinetic and mechanistic study

The oxidation of Hg^I by Ce^IV has been studied in aqueous H₂SO₄. A minute amount (10^–6 mol dm^–3) of Os^VIII is sufficient to catalyse the reaction. The active catalyst, substrate and oxidant species are H₂OsO₅, [Hg₂(SO₄)HSO₄]^– and H₃Ce(SO₄)^– ₄, respectively. Possible mechanisms are proposed and the reaction constants involved have been determined.     

Binding interaction and conformational changes of human serum albumin with ranitidine studied by spectroscopic and time-resolved fluorescence methods

This study was designed to examine the interaction of histamine H₂-receptor antagonist drug ranitidine (RTN) with human serum albumin by multi-spectroscopic methods. The experimental results showed the involvement of dynamic quenching mechanism which was further confirmed by lifetime spectral studies. The binding constants (K _a) at three temperatures (288, 298, and 308 K) were 2.058 ± 0.020, 4.160 ± 0.010 and 6.801 ± 0.011 × 10⁴ dm³ mol^?1, respectively, and the number of binding sites (m) were 1.169, respectively; thermodynamic parameters ΔH ⁰ (44.152 ± 0.047 kJ mol^?1), ΔG ⁰ (?26.214 ± 0.040 kJ mol^?1), and ΔS ⁰ (236.130 ± 0.025 J K^?1 mol^?1) were calculated. The distance r between donor and acceptor was obtained (r = 3.40 nm) according to the Förster theory of non-radiative energy transfer. Synchronous fluorescence, CD, AFM and 3D fluorescence spectral results revealed the changes in secondary structure of the protein upon interaction with RTN. A molecular modeling study further confirmed the binding mode obtained by the experimental studies.     

Oxidation of Acyclovir by a Cuprate(III) Periodate Complex in Aqueous Alkaline Media: A Kinetic and Mechanistic Approach

The oxidation of acyclovir by diperiodatocuprate(III) in aqueous alkaline media, at a constant ionic strength of 0.01 mol?dm^?3, was studied spectrophotometrically at 25?°C. The reaction between acyclovir and DPC in alkaline media exhibits 1:4 stoichiometry (acyclovir:diperiodatocuprate(III)). The main oxidation products were identified by a spot test, along with infrared and liquid chromatography mass spectral studies. The oxidation reaction is first order with regard to the diperiodatocuprate(III) concentration, but has less than unit order in the acyclovir concentration and negative fractional orders in the periodate and alkali concentrations. Intervention of free radicals was observed in the reaction. The oxidation reaction in alkaline media was shown to proceed via a diperiodatocuprate(III)?Cacyclovir complex, which decomposes slowly in a rate determining step followed by subsequent fast steps to give the products. A suitable mechanism is proposed for these observations. The reaction constants involved in the different steps of the mechanism were calculated. The activation parameters with respect to the slow step of the mechanism, along with the thermodynamic quantities, were determined and discussed.     

Study on the interaction between antibacterial drug and bovine serum albumin: A spectroscopic approach

The binding of sulfamethoxazole (SMZ) to bovine serum albumin (BSA) was investigated by spectroscopic methods viz., fluorescence, FT-IR and UV–vis absorption techniques. The binding parameters have been evaluated by fluorescence quenching method. The thermodynamic parameters, ΔH°, ΔS°and ΔG° were observed to be −58.0 kJ mol⁻¹, −111 J K⁻¹ mol⁻¹ and −24 kJ mol⁻¹, respectively. These indicated that the hydrogen bonding and weak van der Waals forces played a major role in the interaction. Based on the Forster's theory of non-radiation energy transfer, the binding average distance, r, between the donor (BSA) and acceptor (SMZ) was evaluated and found to be 4.12 nm. Spectral results showed the binding of SMZ to BSA induced conformational changes in BSA. The effect of common ions and some of the polymers used in drug delivery for control release was also tested on the binding of SMZ to BSA. The effect of common ions revealed that there is adverse effect on the binding of SMZ to BSA.     

Oxidation of diclofenac sodium by diperiodatoargantate(III) in aqueous alkaline medium and its determination in urine and blood by kinetic methods

The kinetics and oxidation of diclofenac sodium (DFS) by diperiodatoargentate(III) (DPA) in alkaline medium at 298 K and at a constant ionic strength of 0.60 mol dm^?3 were studied spectrophotometrically. The oxidation products were [2‐(2,6‐dicloro‐phynylamino)‐phenyl]‐methenol and Ag(I), identified by LC‐ESI‐MS and IR spectral studies. The reaction between DFS and DPA in alkaline medium exhibits 1:1 stoichiometry. The reaction is first order in [DPA] and has a less than unit order dependence each in [DFS] and [alkali]. Increasing concentrations of IO^?₄ retard the reaction. The active species of DPA proposed to be monoperiodatoargentate(III), and a mechanism is suggested. The rate constants involved in the different steps of the mechanism were determined and are discussed. The activation parameters with respect to a rate‐limiting step of the mechanism were determined. The thermodynamic quantities were also determined. Using the oxidation of DFS by DPA, DFS was analyzed by kinetic methods in urine and blood sample. The proposed method enables DFS analysis in the range from 5.0 × 10^?5 to 5.0 × 10^?3 mol dm^?3. © 2010 Wiley Periodicals, Inc. Int J Chem Kinet 42: 336–346, 2010     

Kinetics and mechanism of palladium(II) catalyzed chromium(VI) oxidation of mercury(I) in aqueous sulphuric acid

The Cr^VI oxidation of Hg^I in an aqueous acid medium occurs to a modest extent only in presence of Pd^II and in H₂SO₄ above ca. 0.20 mol dm^–3. The reaction is first order in [Cr^VI] in the presence of Pd^II catalyst. The order in [Hg^I] is less than unity, whereas that in [Pd^II] is unity. Increase in [H₂SO₄] accelerates the reaction rate. The added products, Cr^III and Hg^II, do not significantly effect the reaction rate. A mechanism involving HCrO₄ ^– and PdCl⁺ as the reactive species of oxidant and catalyst respectively, is proposed. The reaction constants involved in the mechanism have been evaluated.