Spectrophotometric Determination of Etilefrine Hydrochloride,Prenalterol Hydrochloride and Ritodrine Hydrochloride in pharmaceutical dosage form Through Nitrosation and Subsequent Copper Chelation

Abstract

A colorimetric method is proposed for the determination of etilefrine hydrochloride, prenalterol hydrochloride and ritodrine hydrochloride, and their dosage forms. The proposed method depends on nitrosation of the phenolic drugs with sodium nitrite in acidic medium with subsequent chelation by copper (II) ions resulted in the formation of stable red color copper chelate which shows a maximum absorbance at 510, 460 and 520 nm for etilefrine, prenalterol and ritodrine chelate, respectively. The experimental conditions leading to optimum color stability and intensity were studied. The proportions of the reactants and the stability constant for the copper chelates were determined. The copper chelates obey Beer's law and their absorbance were used for the determination of the three drugs in their pharmaceutical dosage forms. To confirm the validity of the proposed method, recovery studies were carried out using the standard addition method. At the same time, the results of the applications of the method to the assay of the tested drugs in their commercial preparations were compared statistically with either an official or a published method. The proposed method demonstrate high percentage of recoveries with good accuracy and precision.     

Sensitive Spectrophotometric Determination of Some Dibenzazepine Drugs with Diazotized P-Phenylenediamine Dihydrochloride

ABSTRACT

A simple, sensitive and selective spectrophotometric procedure was developed for the determination of imipramine hydrochloride, desipramine hydrochloride, clomipramine hydrochloride and trimipramine maleate belonging to dibenzazepine class of drugs. The method is based on the interaction of diazotized p-phenylenediamine dihydrochloride with the drug in sulphuric acid medium. The resulting chromophore was measured at 565 nm, and was stable for about 2.5 hr. The commonly encountered excipients and additives do not interfere with the determination. Dibenzazepine drugs can be determined in the range of 0.1-4.0 μg/ml, with a relative standard deviation of 1.92% for ten replicate measurement of 2.0 μg/ml dibenzazepine drugs. Results from the analysis of preformulations and commercial tablets by this procedure agree well with those of the official method.     

Colorimetric Determination of Some Important Hydrazine Derivatives

ABSTRACT

A simple and rapid colorimetric method for the determination of isoniazid, iproniazid phosphate, phenylhydrazine hydrochloride and hydrazine hydrate is described. The method is based on the formation of a Schiff base when these compounds react with 4-dimethylaminocinnamaldehyde and measurement of the condensed products at 370–555nm. The procedure has been successfully applied to the assay of the pharmaceutical preparations containing the studied drugs and hydrazine, and phenylhydrazine mixture, and the results are compared to the official methods. All the different experimental conditions are studied and incorporated into the procedure.     

New,simple, and validated UV-spectrophotometric method for the estimation of some beta blockers in bulk and formulations

A sensitive, extraction, derivatization, evaporation and complexation-free, direct spectrophotometric method is developed for the determination of some anthypertensive drugs such as acebutolol hydrochloride (ACH), atenolol (ATE), and propranolol hydrochloride (PRH) in bulk and pharmaceutical formulations. The optimum conditions for the analysis of aqua solutions of drugs are established. The method permits the determination of ACH, ATE, and PRH over a concentration range of 37.3–111.9, 53.3–213.1 and 14.8–51.8 μg/mL, respectively. Detection and quantification limits are calculated. The obtained results showed good recoveries of 99.60, 99.20 and 99.80% with relative standard deviations of 0.82, 0.79 and 1.70% for ACH, ATE, and PRH, respectively. The repeatability and reproducibility of the drugs for aqua media are determined. Precision and accuracy of the developed methods are used for the recovery studies. The proposed method is applicable for the assay of the three drugs under investigation in dosage forms and the results are in good agreement with those obtained by the literature method. The text was submitted by the author in English.     

Spectrophotometric methods for sertraline hydrochloride and/or clidinium bromide determination in bulk and pharmaceutical preparations

A spectrophotometric procedure for the determination of sertraline hydrochloride (Sert) and/or clidinium bromide (Clid) in bulk sample and in dosage forms was developed. The purpose of this work was to develop a rapid, simple, inexpensive, precise, and accurate visible spectrophotometric method. The procedure is based on formation of an ion-pair complex by their reaction with bromocresol green (BCG), bromophenol blue (BPB), and bromothymol blue (BTB) in buffered aqueous solution at pH 3. The colored products are extracted into a polar solvent and measured spectrophotometrically at the optimum λ_max for each complex. Optimization of different experimental conditions is described. Regression analysis of Beer-Lambert plots showed good correlation in the concentration range of 1–30 μg mL⁻¹. The apparent molar absorptivity, Sandell sensitivity, detection and quantification limits were calculated. For more accurate analysis, Ringbom optimum concentration range of 2–27 μg mL⁻¹ was used. The developed methods were successfully applied for the determination of sertraline hydrochloride and clidinium bromide in bulk in pharmaceutical formulations without any interference from common excipients. The procedure has the advantage of being highly sensitive and simple for the determination of the studied drugs, weak UV-absorbing compounds.     

Flow Injection Chemiluminescence Determination of Difenidol Hydrochloride Using N-Chlorosuccinimide-Dichlorofluorescein Reaction

Abstract

A flow injection method combined with chemiluminescence detection was described for the determination of difenidol hydrochloride. Strong chemiluminescence was recorded when difenidol hydrochloride was added into the reaction mixture of N-chlorosuccinimide with dichlorofluorescein in alkaline medium. The experimental conditions that affected the chemiluminescence signal, including the concentrations of reactants, the reaction medium, and the instrumental parameters, were carefully optimized. Under the optimum experimental conditions, the enhanced chemiluminescence intensity was linear related to the concentration of difenidol hydrochloride in the range of 4.0 × 10^?9 to 4.0 × 10^?7 g/ml. The detection limit for difenidol hydrochloride was 7 × 10^?10 g/ml, and the sample throughput was 90/h. The relative standard deviation was 2.5% for 5.0 × 10^?8 g/ml difenidol hydrochloride solution (n = 11). The interference of common inorganic ions, excipients, and additives used in pharmaceutical preparation was studied, which showed the method has higher tolerance limit for these substances and has good selectivity. As a preliminary application, the method was applied to the determination of difenidol hydrochloride in tablets, and the satisfactory results were achieved.     

Flow Injection Analysis of Some Phenolic Sympathomimetic Drugs

ABSTRACT

A new, rapid and economical flow-injection (FI) method for deter-mining some phenolic sympathomimetic drugs is proposed. These drugs are etilefrine hydrochloride (ET), fenoterol hydrobromide (FT), hexoprenaline sulphate (HP), orciprenaline sulphate (OP) and reproterol hydrochloride (R.T). The determination is based on the reaction of the studied phenolic sympathomimetic drugs with 4-aminoantipyrine (4-AAP) and potassium hexacyanoferrate (III). The chemical reaction variables and also the FI variables, were optimized on the basis of sensitivity, sampling rate and reagent consumption. The proposed technique was applied to the analysis of pure raw materials in concentrations ranging from 2-20 μg.ml^?1 in case of ET, 4-30 μg.ml^?1 in case of FT and OP and from 8-50 μg.ml^?1 in case of HP and RT. Samples can be introduced at rates of about 130 per hour. The suggested procedure retained its accuracy and precision when applied to the analysis of pharmaceutical dosage forms containing the corresponding drugs, as judged by the RSD (%) and students' test. The results of the analysis were found to agree statistically with those obtained by applying either the official or the referee methods. Furthermore, the validity of the results was assessed by applying the standard addition technique.     

Spectrophotometric Determination of Some Cardiovascular Drugs Using P-Chloranilic Acid

Abstract

A simple and sensitive spectrophotometric method for the assay of some cardio-vascular drugs is described. The method is based on the interaction of the drug and p-chloranilic acid (p-CA) to give a stable and intensively coloured ion-pair salt. The drugs used are quinidine sulphate, prenylamine lactate, dipyridamol, hydralazine hydrochloride, tolazoline hydrochloride and pindolol. The optimum experimental conditions for colour development have been studied. Conformity to Beer's law enabled the determination of these drugs in their pharmaceutical preparations. The assay results are in accord with the pharmacopoeal assay results.     

Sensitive determination of nitrogenous hydrochloride drugs via their reaction with ammonium molybdate

In a hydrochloric acid medium, benzhexol hydrochloride, cyproheptadine hydrochloride, and maprotiline hydrochloride, can react with ammonium molybdate to form ion-association complexes by virtue of electrostatic attraction and hydrophobic interaction which result in a significant enhancement of the resonance light scattering intensity. The maximum scattering wavelengths were found at 364 nm, 364 nm, and 381 nm for benzhexol hydrochloride, cyproheptadine hydrochloride, and maprotiline hydrochloride systems, respectively. Spectral characteristics of the three systems, influencing factors, and optimum conditions were investigated. The reason of resonance light-scattering enhancement and the mechanism of interactions between the drugs and ammonium molybdate were also discussed. Based on the linear relationship between the enhanced intensity of resonance light scattering and the concentration of drugs, a highly sensitive method for the determination of the three drugs was developed, the detection limits being 0.0110 μmol L⁻¹, 0.0038 μmol L⁻¹, and 0.0155 μmol L⁻¹ for benzhexol hydrochloride, cyproheptadine hydrochloride, and maprotiline hydrochloride, respectively. The method was successfully applied to the determination of the investigated drugs in pharmaceutical, serum, and urine samples.     

The Simultaneous Determination of Phenylephrine Hydrochloride,Paracetamol, Chlorpheniramine Maleate and Dextromethorphan Hydrobromide in Pharmaceutical Preparations

A new rapid and sensitive method has been developed and validated for the simultaneous determination of phenylephrine hydrochloride, paracetamol, chlorpheniramine maleate and dextromethorphan hydrobromide in pharmaceutical preparations. The separation was achieved on a C18 column using a gradient mobile phase of acetonitrile–sodium perchlorate (pH 3, 0.01 M) at a flow rate of 1.4 mL min⁻¹. Detection was at 204 nm. Pseudoephedrine hydrochloride was selected as internal standard. The recovery of the drugs ranged from 97.8 to 100.9%. Central composite design was used during validation to calculate method robustness and the percentage of sodium perchlorate, temperature and flow rate were investigated as factors. The method was found to be applicable for the determination of the four compounds in sugar-coated tablets.

     

Simultaneous Determination of Hydrochlorothiazide and Propranolol Hydrochloride in Tablets by High-Performance Liquid Chromatography

Abstract

A simple and stability indicating HPLC procedure is described for the simultaneous determination of hydrochlorothiazide and propranolol hydrochloride in tablet formulations. Potential degradation products of both drugs and synthesis impurities of hydrochlorothiazide were separated, making the determination stability indicating for both drugs and selective for hydrochlorothiazide. All compounds were chromatographed on a cyanopropylsilane column, eluted with a 15:85 mixture of acetonitrile: 0.05 M ammonium phosphate (pH 3.0) and detected at 290 m. Excellent interlaboratory precision and recovery data were obtained. Linearity studies were carried out using peak area measurements. Detector response to the concentration of each drug was confirmed. The method was applied to dosage forms containing 25 mg of hydrochlorothiazide and 40 or 80 mg of propranolol hydrochloride.     

Simultaneous Determination of Dipyrone and Papaverine in Pharmaceutical Formulation using PLS Regression and UV Spectrophotometry

Abstract

A combination of sodium dipyrone and papaverine hydrochloride is used as an analgesic and antispasmodic drug. A simple and rapid procedure is proposed for simultaneous determination of these drugs in commercial formulations (Melpaz^®) based on partial least squares (PLS) regression and UV spectrophotometric measurements in the range of 218–300 nm. The calibration set was built with 25 solutions in concentrations ranging from 15.0–35.0 mg ml^?1 for dipyrone and from 0.5–1.5 mg ml^?1 for papaverine in methanol. The relative standard deviation (RSD) was 1.05% for dipyrone and 1.55% for papaverine in pharmaceutical formulations. The percent of relative recovery was 95.9% for dipyrone and 95.2% for papaverine. Figures of merit, such as accuracy, precision, sensitivity and adjust were also determined. The methodology was validated by using an independent method, based on high performance liquid chromatography (HPLC).     

Application of Membrane-Selective Electrodes for the Determination of Pioglitazone Hydrochloride in the Presence of Its Acid Degradant or Metformin Hydrochloride in Tablets and Plasma

Abstract

Polyvinyl chloride (PVC) membrane sensors for the determination of pioglitazone hydrochloride (PIO) and metformin hydrochloride (MET) were described by using the ion association complexes between these drugs with either sodium tetraphenyl-borate (TPB) or ammonium reineckate (RNC) counter ions. The performance characteristics of the sensors were evaluated according to IUPAC recommendations, reveal a fast, stable and linear response over the concentration range 3.162 × 10^?5 ? 1 × 10^?2 M for PIO and 1 × 10^?3 ? 1 × 10^?1 M for MET. The sensors are used for determination of PIO and MET in tablets and plasma. The developed method was found to be simple, accurate and precise when compared with the reported method.     

A Sensitive Spectrophotometric Method for the Determination of Some Imidazoline Derivatives by 2,6-Dichlorophenol-Indophenol

Abstract

A new and highly sensitive method is presented for the spectrophotometric determination of four imidazoline derivatives: antazoline hydrochloride, tolazoline hydrochloride, xylometazoline hydrochloride and naphazoline nitrate. The method is based on the reaction of the corresponding drug base with 2,6 - dichlorophenol -indophenol (DGPIP) in chloroform to give a blue chromogen exhibiting a maximum at 588 - 603nm. The method could be applied for the quantitative determination of the above drugs either pure or in their pharmaceutical preparations (tablets and nasal drops). The results obtained are accurate and have good reproducibility.     

Spectrophotometric and Indirect Determination of Lincomycin by Atomic Absorption Spectroscopy (AAS)

Abstract

The reaction of lincomycin with cupric ions in alkaline medium was taken as a basis for the colorimetric and indirect atomic absorption spectrometric (AAS) determination of lincomycin hydrochloride.

The AAS procedure was based on the extraction of copper-lincomycin complex at pH 11, into n-butanol. The copper content in this extract was determined by AAS. The response was linear for up to 30 μg ml^?1 of lincomycin. The method is accurate, sensitive and simple.

The proposed methods were applied to pharmaceutical preparations with fine accuracy.     

Colorimetric and Bromometric Determination of Pirbuterol Hydrochloride

Abstract

Two proposed methods are reported for the quantitation of pirbuterol hydrochloride, namely, (i) colorimetric and (ii) titrimetric methods. The colorimetric method is based on coupling betweem diazotized sulphanilamide and pirbuterol hydrochloride. Under the optimum conditions studied, the coupling product exhibits a maximum at 440 nm. Linear relation between absorbance, A, and concentration of pirbuterol hydrochloride is in the range 5–40 μgml^?1. The mean percentage obtained for capsules (Exirel^R ?15 mg) was 100.8 ± 0.7 whereas mean percentage recovery obtained for the authentic drug was 100.5 ± 0.8.

The titrimetric procedure involves bromination of authentic pirbuterol in acid medium and residual titration of excess bromine. The stoichiometry of the reaction was investigated and infra-red analysis, of the bromoderivative was carried out. When applied to capsules the bromometric method gave mean percentage of 100.18 ± 2.25.     

Spectrophotometric determination of some phenothiazine drugs using chloramine-T-iodine-starch

A simple, accurate, and sensitive spectrophotometric method for the determination of promethazine hydrochloride (PMH), prochlorperazine maleate (PCPM), trifluoperazine hydrochloride (TFPH), trimeperazine tartrate (TMT), fluphenazine dihydrochloride (FH), and trifluopromazine hydrochloride (TPH) is described. The method is based on the oxidation of the studied drugs by a known excess of chloramine-T in a hydrochloric acid medium and subsequent determination of the unreacted oxidant by interacting it with iodide in the same acid medium. Liberated iodine subsequently reacts with starch to form a stable starch-iodine complex. The reacted oxidant corresponds to the drug content. The colored complex exhibits a maximum absorption at 590 nm. The apparent molar absorptivity and Sandell sensitivity values are in the range 4.07 × 10⁴ − 1.18 × 10⁵ L/mol cm and 45.00−95.00 ng/cm², respectively. The proposed method has been applied to the assay of phenothiazine drugs in pure and dosage forms. The reliability of the analysis was established using parallel determination by the reference method. The text was submitted by the authors in English.     

Flow‐Injection Chemiluminescence Analysis of Cloperastione Hydrochloride

Abstract

A new chemiluminescence (CL) reaction was observed when cloperastine hydrochloride was injected into the reaction mixture after the CL reaction of Ce(IV) and sodium sulfite finished. A new flow injection CL method for the determination of cloperastine hydrochloride was established based on the CL reaction. The relative standard deviation (RSD) for the determination of cloperastine hydrochloride was 1.3% (n=11, c=1.0×10^?6 g/mL). The CL intensity responded linearly to the concentration of cloperastine hydrochloride in the range 2.0×10^?7～2.0×10^?5 g/mL (r=0.9962). The detection limit was 5×10^?8 g/mL cloperastine hydrochloride. The method had been applied to the determination of cloperastine hydrochloride in tablets with satisfactory results.     

Application of the Coupled Redox and Complexation Reactions to Flow Injection Spectrophotometric Determination of Promazine

Abstract

A flow injection (FI) spectrophotometric method is proposed for the determination of promazine hydrochloride. The method is based on the coupled redox - complexation reactions which proceed in the promazine-iron(III) and 1,10-phenantroline system. A linear calibration graph was obtained between 2–12 ppm of promazine hydrochloride with a sampling rate of 163 samples h^?1. The proposed method was applied to the determination of promazine in pharmaceuticals.     

Spectrophotometric Determination of Some Fluoroquinolone Derivatives in Dosage Forms and Biological Fluids Using Ion‐Pair Complex Formation

Abstract

A simple, rapid, sensitive, and reproducible procedure for assaying norfloxacin (NOR), ciprofloxacin (CIP), and ofloxacin (OFL) was investigated. The procedure is based on the reaction of selected drugs with Sudan II (I), Congo red (II), and Gentian violet (III) in universal buffer to give soluble ion‐pair complexes. The effects of various parameters have been studied. Beer's law plots were obeyed in the concentration ranges 0.5–11 µg ml^?1, whereas Ringbom optimum ranges were 0.7–9.5 µg ml^?1. The apparent molar absorptivity (6.4×10⁴ L mol^?1 cm^?1), Sandell sensitivity (4.99 ng cm^?2), detection (0.13 µg ml^?1), and quantification (0.44 µg ml^?1) limits were calculated. The relative standard deviation for ten determinations, for samples containing 4.0 µg ml^?1, was found to be 1.40%. The influence of commonly employed excipients in the determination of the studied drugs was examined. There was no interference from degradate product results from thermal and hydrolytic treatments. The results obtained by the proposed procedure were statistically validated. The developed procedure was successfully applied to the determination of the studied drugs in dosage forms and biological fluids.