Exactly 1 mg of ciprofloxacin was dissolved in 1 mL of 0 1 N hydr

Exactly 1 mg of ciprofloxacin was dissolved in 1 mL of 0.1 N hydrochloric acid. Then 0.5 mg of zinc Alectinib cost sulphate crystals was added slowly with constant stirring. Then the solution was diluted to 80 mL and the pH of the solution adjusted to 8 using 0.1 N sodium hydroxide. Then this solution was made up to 100 mL. From this stock solution further dilutions were made for subsequent experiments. The same procedure was followed for the preparation of cipro (market sample)–zinc complexes. A double beam UV–Vis (Jascow-500) spectrophotometer with 1 mm optical path length quartz cells was used for all absorbance measurement in the range of 200–600 nm. Fourier transform infrared spectra (FT-IR) were recorded BKM120 research buy using Nicolet

6700 (Thermo Electronic Corporation, USA) and the electrochemical behaviour of this complex were measured using

Electrochemical work station (CHI650C instruments, USA). The cyclic voltammogram was scanned in the potential range −1.2 V–2.0 V versus Ag/AgCl at a sweep rate 50 mVs−1. UV–Vis spectral studies reveal the formation of zinc complex with ciprofloxacin from Fig. 2. Pure ciprofloxacin shows absorbance at 271 nm, 316 nm and 323 nm which is supported by Thangadurai et al reports.14 There is a bathochromic shift observed from 271 nm to 277 nm after the complexation and changes in the absorbance peaks from 316 nm to 323 nm and from 329 nm to 333 nm. The IR spectra of quinolones are almost indicative in the region 1800–1300 cm−1. The characteristic band for Isotretinoin the γ(C=O) vibration of the carboxylic group in ciprofloxacin hydrochloride hydrate is at 1707 cm−1. The IR spectra of complex (Fig. 3) shows no band for the γ(C=O) of the carboxylic group in the region 1800–1300 cm−1 as carboxylic group has been deprotonated. The voltammetric behaviour of ciprofloxacin (Fig. 4) reveals one oxidation peak potential at 1240 mV and two reduction peaks at 450 mV and 50 mV in reverse scan. The formation of anodic peak is due to the oxidation of secondary amine. The first and second reduction peaks are due to the reduction of oxidized form of amine and the reduction

of C=O group respectively. Fig. 5 shows the voltammogram of ciprofloxacin–zinc (II) complex on glassy carbon surface. At pH 8, the forward scan shows the oxidation potential starting at about 1440 mV and no reduction peak. This is due to the oxidation of complex and potential also different from later one. Since carboxylic group involved in the formation of metal complex, no reduction peak is observed. From this report, the formation of complex is confirmed. Based on the above results, the pattern of the complex formation is proposed in Scheme 1. Thangadurai et al reported the similar mechanistic scheme for complexation of iron with ciprofloxacin.14 The complexation procedure was applied for the analysis of market samples which were purchased and the Fig. 6 explains their purity.

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