Fluorimetric determination of mebendazole and flubendazole in pharmaceutical dosage forms after alkaline hydrolysis

The selective and very sensitive fluorimetric determination of mebendazole and flubendazole is based on alkaline hydrolysis and adsorption on Whatman 42 filter paper. Limits of detection are 0.1 μg ml^?1 and 0.5 μg ml^?1, respectively, with linear response sponse up to 10 μg ml^?1 and 50 μg ml^t?1. The fluorescence produced is very stable (λ_em = 460 nm) and the method is applicable to anthelmintic pharmaceutical preparations.     

Pharmacokinetics and Tissue Distribution Study of Tryptanthrin in Rats by RP-HPLC with DAD Detector

A simple RP-LC-UV method was established for the determination of tryptanthrin in plasma and different tissues of rats. The separation was achieved by HPLC on a C₁₈ column with a mobile phases composed of acetonitrile?Cwater (47:53, v/v), UV detection was used at 251?nm. Good linearity was found between 0.0183?C1.1712???g?mL^?1 (r ²?=?0.999) for plasma and 0.0937?C1.7568???g?mL^?1 for the tissue samples, respectively (r ²????0.9932). The intra- and inter-day precisions expressed as the relative standard deviation for the method were 0.92?C6.01 and 1.06?C9.11?%, respectively. The relative recoveries of tryptanthrin ranged from 95.26 to 97.89?% for plasma and 82.55 to 114.99?% for tissue homogenates (except heart). The developed method was successfully applied to the pharmacokinetics and tissue distribution research after orally administration of a 56-mg?kg^?1 dose of tryptanthrin to healthy SD rats. The main pharmacokinetics distribution results showed that liver, lung, small intestine, and large intestine were the major distribution tissues of tryptanthrin in rats, and that tryptanthrin had difficulty in crossing the blood?Cbrain barrier.     

Fourth Order Derivative Spectrophotometric Determination of Benzyl Alcohol in Piroxicam Injections

Piroxicam is a drug with analgesic and anti‐inflammatory properties. It is present in numerous pharmaceutical preparations. Injectable forms usually contain benzyl alcohol as an excipient, which is used as a blocking anesthetic (4%) and an antiseptic (4–10%). In this work, spectrophotometric methodology was used in order to determine benzyl alcohol in piroxicam injectable formulations by applying the fourth derivative method adopting the zero‐crossing technique. The results obtained show that the method has significant advantages over other reported methods and is appropriate for routine pharmaceutical analysis. The method showed excellent linearity in the range of 2–100 μg mL^?1 with limit of detection (S/N = 3) 0.07 μg mL^?1 (6.47 × 10^?7 M). The proposed method could be applied successfully for the determination of benzyl alcohol in injectable formulations with average % recovery of 100 ± 0.61.     

Spectrophotometric Methods for the Determination of Acediasulfone in Mixture with Cinchocaine

Abstract

Derivative spectrophotometry techniques (ratio‐spectra first derivative and zero‐crossing first derivative) were described for simultaneous determination of acediasulfone and cinchocaine. Acediasulfone was also determined via the formation of a colored product as a result of its reaction with p‐dimethylaminobenzaldehyde. In the ratio‐spectra first derivative method, the measurements were taken at 310 and 233.9 nm for acediasulfone and cinchocaine, respectively. By the zero‐crossing first derivative method, lines of regression were taken at 318 and 233 nm for acediasulfone and cinchocaine, respectively. In the colorimetric method, absorbance measurements were obtained at 452 nm. Acediasulfone showed linearity over concentration ranges 2–14 µg/ml, 2–16 µg/ml, and 12–60 µg/ml for ratio‐spectra first derivative, zero‐crossing first derivative, and colorimetric methods, whereas cinchocaine showed linearity over concentration ranges 1–10 µg/ml and 2.28–16 µg/ml for ratio‐spectra first derivative and zero‐crossing first derivative techniques. The proposed methods proved to be specific and accurate for the analysis of the cited drugs in laboratory‐prepared mixtures and dosage form. The obtained results agree statistically with those obtained by reference methods.     

Cathodic stripping voltammetry of pipemidic acid and ofloxacin in pharmaceutical dosages and human urine

Sensitive cathodic stripping voltammetric methods have been developed for two quinolone antibacterial drugs, pipemidic acid (PIP) and ofloxacin (OFL) using hanging mercury drop electrode as working electrode vs. Ag/AgCl reference electrode. The methods were developed for the determination of drugs individually as well as simultaneously. 0.1 M and 0.01 M hydrochloric acid was used as medium for PIP and OFL, respectively, 0.1 M potassium chloride was used as base electrolyte. Reduction waves were observed for PIP within ?700 mV to ?800 mV and for OFL within ?1100 mV to ?1200 mV. Linear calibration ranges for PIP and OFL were observed within 10–100 μg ml^?1 with detection limits of 50 ng ml^?1 and 1 μg ml^?1, respectively. Relative standard deviations (RSD) for the analysis of 10 gµg ml^?1 of PIP and OFL (n = 6) were 0.5% and 1.4%, respectively. The presence of glucose, lactose, sorbitol, gum arabic, starch, magnesium stearate, methylparaben and propylparaben did not affect the determinations of both PIP and OFL. The methods were used for the analysis of pharmaceutical preparations and the results indicated relative deviation of 0.5–5.5% from labeled values with RSD within 0.49–2.5%. PIP and OFL could also be determined simultaneously, and were determined from spiked human urine.     

Simultaneous Determination of Cobalt and Nickel Using Morpholinedithiocarbamate (MDTC) as Reagent by First and Second Derivative Spectrophotometry

A selective and sensitive derivative method has been proposed for the simultaneous determination of trace amounts of Co(II) and Ni(II) with morpholinedithiocarbamate (MDTC) in the presence of sodium lauryl sulphate (SLS). The molar absorption coefficients of the 1:2 complex of Co(II) and Ni(II) at 326 nm and 322 nm are 2.248 × 10⁴ and 2.505 × 10⁴ L mol^?1 cm^?1 for zero order. The analytical sensitivity for the second derivative of Co(II) and Ni(II) complexes are 0.0044 μg mL^?1 and 0.0060 μg mL^?1. The developed derivative procedure, using the zero‐crossing technique, has been successfully applied for the analysis of Co(II) and Ni(II) simultaneously in different alloy samples.     

Simultaneous Determination of Nickel(II) and Copper(II) by Second‐Derivative Spectrophotometric Method in Micellar Media

A second‐derivative spectrophotometric method based on zero‐crossing over technique is developed in simultaneous determination of copper(II) and nickel(II) ions. Methylthymol blue (MTB) as a chromogenic reagent and cetyltrimethylammonium bromide as a surfactant were used, and measurements were carried out in buffered solution at pH 6 and at a temperature of 25 °C. The amplitude of derivative spectra was measured at wavelengths of 631.9 and 587.7 nm for the simultaneous determination of Ni²⁺ and Cu²⁺, respectively. Linearity was obtained in the range of 0.5–5.0 μg mL^?1 for both ions in the presence of 0.0–5.0 μg mL^?1 of the other ion as an interfering ion. IUPAC detection limits for Cu²⁺ and Ni²⁺ ions were obtained at 0.48 and 0.43 μg mL^?1, respectively. The proposed procedure has been applied successfully for the simultaneous determination of copper and nickel in synthetic binary mixtures and real samples.     

Chiral Determination of Salbutamol, Salmeterol and Atenolol by Two-Dimensional LC–LC: Application to Urine Samples

A heart-cut two-dimensional high-performance liquid chromatography method for enantiomeric determination of salbutamol, salmeterol and atenolol in urine is presented. It involves the use of two separations in a liquid chromatography?Cliquid chromatography achiral?Cchiral coupling. Target compounds were previously separated in a primary column (Kinetex? HILIC, 2.6???m, 150?×?2.1?mm I.D.) with a mixture of MeOH:ACN:ammonium acetate buffer (5?mM, pH 6) 90:5:5 (v/v/v) as mobile phase at a flow rate of 0.40?mL?min^?1. Enantiomeric separation was carried out by transferring peak of each compound through a switching valve to a vancomycin chiral column (Chirobiotic? V, 2.6???m, 150?×?2.1?mm I.D.) using MeOH:ammonium acetate buffer (2?mM, pH 4) 97:3 (v/v) as mobile phase at a flow rate of 0.50?mL?min^?1. Ultraviolet detection was done at 227?nm. The method was applied to determine target analytes in urine samples after enzymatic hydrolysis with ??-glucuronidase from Helix pomatia, followed by a solid-phase extraction procedure using Isolute^? HCX mixed-mode cartridges. Extraction recoveries ranged from 82 to 90?% in urine samples. Detection limits were 0.091?C0.095???g for each enantiomer of atenolol and between 0.058 and 0.076 and 0.18?C0.14???g for enantiomers of salbutamol and salmeterol, respectively (3?mL of urine). Linearity ranges were between 0.5 and 10???g?mL^?1. Intraday and interday reproducibilities of enantiomeric ratio and enantiomeric fraction, expressed as relative standard deviation, were between 1.9 and 9.0?%. The optimized method was successfully applied to the analysis of urine samples obtained from excretion studies in volunteers and in freeze-dried urine samples, containing urinary components with MW?<?10,000 and components with MW?>?10,000, spiked with different amounts of studied drugs.     

Spectrophotometric and Spectrofluorimetric Determination of Famotidine and Ranitidine Using 1,4-Benzoquinone Reagent

ABSTRACT

Spectrophotometric and spectrofluorimetric methods were adopted for the analysis of Famotidine and Ranitidine depending on their reaction with 1,4 Benzoquinone reagent at pH 5.2 and 5.6, respectively. The absorbances of the resulting condensation products were measured at 502 and 508 nm for Famotidine and Ranitidine, respectively. Concentrations adhering to Beer's law were from 40-160 μg.ml^? for Famotidine and from 20-100 μg.ml^? for Ranitidine.

Furthermore the resulting condensation products exhibited fluorescence at 665 nm when excited at 290 nm and the calibration graphs were rectilinear from 0.4-1.4 μg.ml^? for Famotidine and from 0.21 μg.ml^? for Ranitidine.

Different parameters affecting these reactions were thoroughly studied. Also these methods were applied to the pharmaceutical preparations and the results were satisfactory. The validities of the methods were ascertained by the standard addition technique revealing fine results in consideration to the mean recovery percent and standard deviation.

The spectrofluorimetric method was a hundred times more sensitive then the spectrophotometric method. The proposed methods were sensitive, accurate, and precise as statistically compared with the official methods of analysis of Famotidine and Ranitidine.     

Reverse-FIA with spectrophotometric detection method for determination of vitamin C

Simple reverse flow injection analysis (rFIA) manifold with spectrophotometric detection was developed for an indirect determination of ascorbic acid. Parameters such as stability, accuracy and precision were established for the method and evaluated statistically to assess the applications of the method. Ascorbic acid in this procedure accelerates dediazoniation reaction of formed diazonium ions; hence its quantity can be determined by monitoring the derivatization product from coupling unreacted diazonium ion with phenol to give an azo dye (coupling reaction). The rFIA design was based on the injection of sodium nitrite into an acidic p-aminoacetophenon carrier stream in which diazonium ion was formed. This ion was inhibited by ascorbic acid stream before coupling with the phenol-Na₂CO₃ stream. Under optimum conditions, ascorbic acid acts in accordance with the Beer??s law at two concentration ranges 0.4?C6.5 ??g ml^?1 (R = 0.9995) and 7.0?C20.0 ??g ml^?1 (R = 0.9949), with detection limits of 0.25 ??g ml^?1. The developed method was applied to the determination of vitamin C in pharmaceutical formulations which produced satisfactory results compared with the standard methods reported in the British Pharmacopoeia.     

Batch and flow-injection determination of ethylenediamine in pharmaceutical preparations

the ethylenediamine/pyridine-2-carbaldehyde/copper(I) system is used in a new spectrophotometric method for the determination of ethylenediamine. The batch procedure involves the formation of an orange chelate between the Schiff's base and copper(I) ions at pH 8.5 (borate buffer) and measurement of the absorbances at 475 nm against water after 10/2-15 min; Beer's law is obeyed over the range 0.5/2-11.2 μg ml^?1 and the molar absorptivity is 6.21 × 10³ l mol^?1 cm^?1. Tolerance limits for different amines [36] and other organic compounds [12] are reported. In the optimized flow-injection system, ethylenediamine (1.4/2-84.6 μg ml^?1 is determined at a sample throughput of 55 h^?1. The method is sensitive and selective and is satisfactory for the determination of the diamine in aminophylline and pharmaceutical preparations (ethylenediamine contents from 0.031 to 3.23%) with relative errors ranging from ?7.4 to +11.1% and relative standard deviations of about 0.65% for both procedures.     

Colorimetric Determination of Propofol in Bulk form,Dosage Form and Biological Fluids

ABSTRACT

Propofol is coupled with 2, 6-dichloroquinone-4-chlorimide (DCQ) in a reaction buffered at pH 9.6 to give a colored product having an analytically useful maximum at 635 nm. The factors affecting the color generation were optimized and incorporated in the procedure. The reacted propofol has a molar absorptivity of 3.9 × 10^?4 L mol^?1 cm^?1, and Beer's law is obeyed for concentrations 1-5 μg ml^?1 with detection limit 0.25 μg ml^?1. The method was found applicable to biological fluids (plasma and urine) spiked with propofol at concentration levels 1-5 μg ml^?1 for plasma and 1-5 μg 0.5 ml^?1 urine (less sensitivity is obtained with urine volumes above 0.5 ml) with detection limits 0.28 μg ml^?1 for plasma and 0.4 μg 0.5 ml^?1 urine. The average recovery for the commercial preparation (1% w/v propofol emulsion intravenous injection for infusion) was 99.54% with an RSD of 1.05%. The method was validated by an adopted HPLC method. The results obtained by the HPLC method for the commercial preparation were statistically compared with the proposed method and evaluated at the 95% confidence limits.     

A Polypyrrole-Based Sorptive Microextraction Coating for Preconcentration of Malathion from Aquatic Media

A new micro-solid phase extraction method was developed by combining solid-phase extraction and stir bar sorptive extraction to benefit from the advantages of both techniques. A polypyrrole coating was electrochemically synthesized on the surface of an already used graphite furnace, employed in electro-thermal atomic absorption spectroscopy. The cylindrical geometry of the graphite tube provided a rather huge surface area, suitable for sorptive extraction. The novel sorbent coating was examined as an extracting medium to isolate malathion. Effects of different parameters such as extraction time, salt concentration, sample volume, desorption solvent and time were investigated and optimized. Under the optimized conditions, the limit of detection and limit of quantification of the developed method were 5 and 20?ng?L^?1, respectively. The calibration curve showed linearity in the range of 0.1?C100???g?L^?1 (R ²?=?0.9968). The precision was evaluated at 0.1 and 1???g?L^?1 concentration levels and relative standard deviations (n?=?3) were found to be 10 and 7%, respectively. The developed method was successfully applied to the extraction of malathion from real river water and tap water samples, and relative recoveries at the spiked level of 0.1???g?L^?1 were 94 and 97%, respectively.     

Spectrophotometric determination of dissolved tri n-butyl phosphate in aqueous streams of Purex process

A spectrophotometric method is developed for the determination of dissolved tri-n butyl phosphate (TBP) in aqueous streams of Purex process used in nuclear fuel reprocessing. The method is based on the formation of phosphomolybdate with added ammonium molybdate followed by reduction with hydrazine sulphate in acid medium. Orthophosphate and molybdate ions combine in acidic solution to give molybdophosphoric (phosphomolybdic) acid, which upon selective reduction (with hydrazinium sulphate) produces a blue colour, due to molybdenum blue. The intensity of blue colour is proportional to the amount of phosphate. If the acidity at the time of reduction is 0.5?M in sulphuric acid and hydrazinium sulphate is the reductant, the resulting blue complex exhibits maximum absorption at 810?C840?nm. The system obeys Lambert?CBeer??s law at 830?nm in the concentration range of 0.1?C1.0???g/ml of phosphate. Molar Absorptivity was determined to be 3.1?×?10^4?L?mol^?1?cm^?1 at 830?nm. The results obtained are reproducible with standard deviation of 1?% and relative error less than 2?% and are in good agreement with those obtained by ion chromatographic technique.     

Novel Reactions for the Simple and Sensitive Spectrophotometric Determination of Traces of Selenium in Environmental Samples

Two rapid, highly sensitive, and selective spectrophotometric methods for the determination of traces of selenium(IV) were studied. The methods are based on either the oxidation of 4‐aminoantipyrine (=4‐amino‐1,2‐dihydro‐1,5‐dimethyl‐2‐phenyl‐3H‐pyrazol‐3‐one; 4‐AAP; 1 ) by selenium in basic medium and coupling with N‐(naphthalen‐1‐yl)ethane‐1,2‐diamine dihydrochloride (NEDA; 2 ?2 HCl) to give a violet derivative 3 or on the oxidation of dopamine hydrochloride (=4‐(2‐aminoethyl)benzene‐1,2‐diol hydrochloride; DPH; 4 ?HCl) by selenium in H₂SO₄ medium and coupling with 1 to yield a red derivative 5 (see Scheme). The violet derivative 3 with λ_max 563 nm is stable for 8 days and the red derivative 5 with λ _max 495 nm for more than a week. Beer's law is obeyed for selenium in the concentration range 0.03–3.5 μg ml^?1 (violet derivative 3 ) and 0.07–2.5 μg ml^?1 (red derivative 5 ), respectively. The optimum reaction conditions and other important analytical parameters were established. Interference due to various non‐target ions were also investigated. The proposed methods, were applied to the analysis of selenium in polluted water, natural water, plant material, soil samples and synthetic mixtures. The results of the analyses were superior in precision to those obtained by reported methods.     

Flow-Injection Chemiluminescence Determination of Fluoroquinolones

ABSTRACT

A new flow-injection CL method was developed for the determination of fluoroquinolones including ofloxacin, norfloxacin, ciprofloxacin and lomefloxacin in pharmaceutical preparations, based on the chemiluminescence reaction of sulphite with cerium(IV) sensitized by these compounds. The linear ranges are 0.04 to 4.0 μg ml^?1 for ofloxacin and 0.4 to 40.0 μg ml^?1 for norfloxacin, ciprofloxacin and lomefloxacin, respectively. The detection limits are 0.016 μg ml^?1 for ofloxacin and 0.16 μg ml ^?1 for norfloxacin, ciprofloxacin and lomefloxacin, respectively. The relative standard deviations (RSD) are 2.1 to 2.6% (n=10) for these fluoroquinolones. The analytical procedure has been applied to the determination of the fluoroquinolones in pharmaceutical commercial formulations. The results are in agreement with those obtained by the official methods.     

Spectrophotometric Determination of Sparfloxacin in Pharmaceutical Preparations by Ternary Complex Formation with Pd(II) and Eosin

Abstract

A simple, sensitive, and direct spectrophotometric method has been developed for the assay of sparfloxacin in bulk and pharmaceutical preparations. The proposed method is based on the formation of ternary complex between an investigated drug, palladium(II) ion and eosin in the presence of methylcellulose as surfactant and acetate buffer of pH 4.2. Spectrophotometrically, under the optimum conditions, the ternary complex showed absorption maximum at 550 nm, with apparent molar absorptivity of 2.69×10⁴ l mol^?1 cm^?1, Sandell's sensitivity of 0.01458 µg ml^?1 and linearity in the concentration range 1.6–16 µg ml^?1. The composition of the ternary complex was studied by Job's method of continuous variation and the result indicated that the molar ratio of SPFX: Pd: eosin is 1∶1∶1. The optimum reaction conditions and other analytical parameters are evaluated. The proposed method was successfully applied for the determination of SPFX in its pharmaceutical product with mean percentage recoveries of 99.71%. The observed data has been subjected to statistical analysis, which revealed high accuracy and precision.     

Spectrophotometric procedure for indirect determination of ranitidine in pharmaceutical formulation using fluorescein sodium

A simple and sensitive spectrophotometric method for the determination of ranitidine hydrochloride (R·HCl) in pharmaceutical formulation is proposed. The procedure is based on the oxidation of R·HCl by bromine, generated in situ by the action of bromate?Cbromide mixture in acid medium, followed by estimation of surplus oxidant by its reaction with fluorescein sodium salt (FL). The decrease in concentration of FL is estimated by measuring its absorbance at ?? _max?=?436?nm. All variables affecting the reaction conditions, such as concentration of NaBrO₃, HCl, NaBr and FL, and reaction time were carefully studied and optimized. The analytical curve was linear in the R·HCl concentration range from 0.3 to 8???g?mL^?1 with a detection limit of 0.13???g?mL^?1. The reliability of the proposed spectrophotometric method was established by parallel determination of pure and dosage forms containing R·HCl, by the reference method and by recovery studies.     

Application of Self-Assembled Monolayers in the Preparation of Solid-Phase Microextraction Coatings

Self-assembled monolayers (SAMs) of polyaminithiophenol (PATP) were used as a covalent bonded coating for solid-phase microextraction (SPME). Thiolated aniline-analog monomers (mixture of 2- and 3-aminothiophenols, 2/3-ATP) were anchored on the gold surface and then electropolymerized. Due to the strong S?CAu bond, thiol-terminated coating on the gold surface was very stable. The proposed covalent bonded coating showed higher mechanical (re-usability up to 100 times) and thermal stability (up to 320???C) than non-covalent bonded polyaniline coating (re-usability up to 20 times and thermal stability up to 250???C). The extraction capability of the proposed fiber for the extraction of five polycyclic aromatic hydrocarbons (PAHs), including phenanthrene, anthracene, pyrene, 9,10-dimethylanthracene and benzo[??]anthracene was examined. The effects of different parameters influencing the extraction efficiency of analytes including extraction temperature, extraction time, ionic strength, stirring rate and sample volume were examined and optimized. Linear ranges of 1?C250???g?L^?1 for phenanthrene and anthracene, and 1?C100???g L^?1 for the other compounds were obtained. Detection limits were in the range of 0.1?C0.32???g?L^?1. Single fiber repeatability and fiber to fiber reproducibility were less than 8.9 and 15.8%, respectively. Seawater sample was analyzed as real sample and good recoveries (81?C108%) were obtained for target analytes.     

Cyclodextrin Enhanced Spectrofluorimetric Determination of Melatonin in Pharmaceuticals and Urine

ABSTRACT

Melatonin forms a 1:1 inclusion complex with methyl-β-cyclodextrin with an association constant of 139 ? 30 M^?1 at 20 °C. The effect of several cyclodextrins and derivatives on the fluorescence spectra of melatonin was studied with a great increase of fluorescence signal when methyl-β-cyclodextrin was employed. Optimal conditions of the method were: [methyl-β-cyclodextrin] = 0.01 M and temperature 20 °C; the pH does not affect the luminescence emission. The linear dynamic range (LDR) was 50-3000 ng ml^?1 and a limit of detection of 10 ng ml^?1 of melatonin was obtained with a relative standard deviation (RSD) of 0.77% (at 0.3 μg ml^?1 level). This simple method was satisfactorily applied to the determination of melatonin in pharmaceutical preparations and urine.