Sequential optimization of a flow injection spectrophotometric method for the assay of chlorpromazine in pharmaceutical preparations

A new simple flow injection spectrophotometric method for the assay of chlorpromazine using cerium(IV) in sulfuric acid media was developed. The oxidized form of the drug was monitored at the maximum absorbance of 526 nm. The optimum conditions were 0.035M sulfuric acid, 3.80 x 10(-3)M cerium(IV), flow rate 4.85 ml/min, coil length 45 cm and sample size 110 mm(3). Optimization was carried out by the modified simplex method. Response surface methodology was employed to investigate the ruggedness of the method. A sampling frequency of 120 hr(-1) was attained. Relative standard deviations for standard sample were usually less than 0.75. The method was applied to the determination of chlorpromazine in proprietary drugs and results were statistically compared with the official British Pharmacopoeia (BP) method.     

Enantioseparation of phenotiazines by affinity electrokinetic chromatography using human serum albumin as chiral selector: application to enantiomeric quality control in pharmaceutical formulations

Nowadays, there is a special interest within the pharmaceutical laboratories to develop single enantiomer formulations and consequently a need for analytical methods to determine the enantiomeric purity of drugs. The present paper deals with the enantiomeric separation of promethazine and trimeprazine enantiomers by affinity electrokinetic chromatography (AEKC)-partial filling technique using human serum albumin (HSA) as chiral selector. A multivariate optimization of the most critical experimental variables in enantioresolution, running pH, HSA concentration and plug length, is carried out to obtain enantioresolution of promethazine and trimeprazine. The estimated maximum and optimum resolution of trimeprazine and prometazine enantiomers (Rs = 1.74 and 2.01, respectively) corresponded to the following experimental conditions: pH 7.5; [HSA] 170 μM and plug length 190 s and pH 7.6; [HSA] 170 μM and plug length 170 s, for trimeprazine and prometazine, respectively. The developed methodologies were applied for the enantiomeric quality control of promethazine and trimeprazine enantiomers in commercially available pharmaceutical formulations. Resolution, accuracy, reproducibility, cost and sample throughput of the proposed methodologies make it suitable for quality control of the enantiomeric composition of promethazine and trimeprazine in pharmaceutical preparations.     

Flow injection method for the assay of the anti-arrhythmic procainamide HCl in drug formulations utilizing statistical optimization techniques

A flow injection spectrophotometric method for the determination of procainamide HCl was explored. The method was based on the oxidation of procainamide HCl with cerium(IV) in sulphuric acid media and subsequent monitoring of the absorbance of the oxidized form of the drug at 480 nm. A sample rate of 250 samples per hour was attained. The procedure was optimized by the Factorial Design at two upper and lower levels of the five parameters sample loop size, flow rate, coil length, sulphuric acid and cerium(IV) concentrations. The latter three indicated high interactions and revealed significance to peak height value therefore optimized by the Super Modified Simplex programme. The optimized FI system with a linear calibration range of 100-600 ppm was found to be adequate and suitable for determination of procainamide HCl in proprietary drugs. A high degree of accuracy of the results was demonstrated by a statistical comparison with those obtained by the British Pharmacopoeia method of the same batch of drugs.     

Flow injection colorimetric method for the assay of vitamin C in drug formulations using tris,1-10-phenanthroline-iron(III) complex as an oxidant in sulfuric acid media

A simple, fast and accurate colorimetric flow injection (FI) method suitable for the assay of vitamin C in drug formulations was proposed. In the method, vitamin C was injected into a flowing stream of iron(III) and then mixed with 1,10-phenanthroline in 0.05M sulphuric acid media. The mixture was allowed to react in a 45-cm long coil and the resulting solution of tris, 1-10-phenanthroline-iron(II) complex was monitored at 510 nm. The method was adopted by fully investigating the kinetics of the reaction and proposing a suitable mechanism. A throughput of 100 samples per hour was achieved with a relative standard deviation of 0.88% for vitamin C concentration range of 100-400 ppm.     

Fluorimetric flow-injection analysis of total amounts of aldehydes in auto exhaust gas and thermal degradation emission gas with cyclohexane-1,3-dione

A simple flow-injection (FI) spectrofluorimetric method for the assay of total volatile aldehydes in auto exhaust gas and emission gas from thermal degradation was developed. Aldehydes, such as formaldehyde, acetaldehyde, propionaldehyde and n-butyraldehyde, reacted with cyclohexane-1,3-dione (CHD) to form more strongly fluorescent compounds. A two-channel flow system was assembled. Distilled water and 0.02% CHD were delivered at 0.75 ml min(-1). The optimum conditions were pH 5 (2.2 M CH(3)COONH(4)-CH(3)COOH buffer solution), reaction temperature 70 degrees C, reaction coil length 0.5 mm i.d. x 7 m, cooling coil length 2 m, sample size 60 microl, excitation and emission wavelengths, 376 nm and 452 nm. Aldehydes in sample gas (10 1) were collected by passing the gas at a flow rate of 0.5 1 min(-1) through two impingers connected in series. 10 ml of methanol was used as an absorbent and diluted sample solution was injected into the carrier stream. The calibration graph was linear in the range 100-1000 ppb. The detection limit was 30 ppb and a sampling frequency of 30 h(-1) was attained. Relative standard deviation for 10 standard formaldehyde solutions (500 ppb) was 1.5%. This rapid and simple FI method was applied to the determination of the total amount of aldehydes, calculated as formaldehyde, in auto exhaust gas and emission gas from the thermal degradation of polymers. The method is useful for monitoring aldehyde emissions and investigating the removal effect of aldehydes from various sources.     

Optimization of high-performance liquid chromatographic parameters for the determination of capsaicinoid compounds using the simplex method.

A high-performance liquid chromatographic method was developed for the analysis of capsaicinoid compounds, the pungent principles of capsicum fruits. A sequential simplex method was applied to optimize the chromatographic response function used to assess the quality of separation by varying the chromatographic parameters. The separation was achieved in 11 min using a C-8 column of 15-cm length and 4.6 mm diameter using a UV detector. A flow rate of 1.15 ml min(-1) at a column temperature of 43.5 degrees C using 63.7% methanol in water gave the most efficient separation. The method was found to be suitable for the determination of the major capsaicinoid compounds in the capsicum samples.     

Evaluation of enantioselective binding of basic drugs to plasma by ACE

The present paper deals with the evaluation of the stereoselective binding of antihistamines (brompheniramine, chlorpheniramine, hydroxyzine, orphenadrine and phenindamine), phenothiazines (promethazine and trimeprazine) and a local anesthetic (bupivacaine) to human plasma proteins. Since all of them are drugs highly bound to proteins, a methodology to determine the bound fraction of each drug enantiomer was proposed. This methodology includes the incubation of samples containing plasma and racemic drug, ultrafiltration of the mixture and the chiral separation of enantiomers in the bound drug fraction using affinity EKC (AEKC)-partial filling technique and HSA as chiral selector. The results shown in this paper represent the first evidence of the enantioselective binding of some antihistamines such as brompheniramine, hydroxyzine, orphenadrine and phenindamine and the phenothiazines, promethazine and trimeprazine, to human plasma proteins. The binding of phenindamine to plasma presented the highest enantioselectivity (ES) (ES = 2.5) followed by trimeprazine (ES = 1.5) and promethazine (ES = 1.4).     

Spectrophotometric determination of ascorbic acid in pharmaceuticals by background correction and flow injection

Background correction has been shown to be an effective and indispensable modification in the spectrophotometric determination of ascorbic acid. The decomposition of ascorbic acid in pharmaceutical samples was carried out by incubation with sodium hydroxide to give products that were insensitive to ultraviolet light. The rapid oxidation in air of ascorbic acid, especially in dilute solutions, was avoided by the use of the flow injection principle for spectrophotometric determination and by employing a carrier stream of an anti-oxidizing nature consisting of 6 micrograms ml(-1) of 2-mercaptoethanol in 0.25% sulphuric acid. The optimized method with a single channel manifold made use of a carrier stream flow rate of 1.1 ml min(-1), an injection volume of 50 microl, a delay coil of 50 cm (0.5 mm i.d.) and detection at 245 nm. The throughput was at least 180 injections h(-1). The proposed flow injection method yielded results for the analysis of 0-20 micrograms ml(-1) of ascorbic acid that were 99-102% (relative standard deviation 0.6% or better) in agreement with those produced by comparable methods involving titration with iodine, chloranil or 2,6-dichlorophenolindophenol [4-(2,6-dichloro-4-hydroxyphenylimino)cyclohexa-2,5-dieno ne], and high-performance liquid chromatography. When the agreement was not good (as low as 14% with respect to the method being compared), this was traced to the presence of substances which are known to interfere in one or other of the methods of comparison.     

Potentiometric determination of bromate using an Fe(III)-Fe(II) potential buffer by circulatory flow-injection analysis.

A method for the potentiometric determination of bromate by circulatory flow injection analysis (CFIA) is described. The procedure involves the use of an Fe(III)-Fe(II) potential buffer solution, which is recycled via a reservoir. The analytical method is based on a linear relationship between the concentration of bromate and a very transient potential change in the electrode potential due to the generation of intermediate bromine during the reaction of bromate with the Fe(III)-Fe(II) potential buffer solution, which also contains NaBr, (NH4)6Mo7O24 and H2SO4. An aliquot (5 microl) of a bromate sample solution was injected into the stream of the potential buffer solution, 100 ml of which was circulated at a flow rate of 1 ml/min; the potential buffer solution stream was then returned to the reservoir after passing through a flow-through redox electrode detector. A potential change due to the reaction of the injected sample with the potential buffer in a reaction coil was measured with the detector in the form of a peak signal. The effects of the bromide, sulfuric acid and Fe(III)-Fe(II) concentrations in the potential buffer, and length of the reaction coil on the peak heights were examined in order to optimize the proposed CFIA method. The analytical sensitivities to bromate were 5.6 mV/microM for 1 x 10(-2) M and 30.9 mV/microM for 1 x 10(-3) M in the concentration of Fe(III)-Fe(II) in a potential buffer solution containing 0.35 M NaBr, 0.2% (NH4)6Mo7O24 and 1 M H2SO4. The detection limit of bromate obtained by a 1 x 10(-3) M Fe(III)-Fe(II) potential buffer solution was 0.02 microM (2.5 ppb). The numbers of repetitive determinations in which the relative sensitivities within 5% were regarded as being tolerated were ca. 4000 and 2000 for the use of only 100 ml of 1 x 10(-2) M and 1 x 10(-3) M Fe(III)-Fe(II) potential buffer solution, respectively.     

Simultaneous determination of sulphide and sulphite by gas-phase molecular absorption spectrometry. Comparative study of different calculation methods

A method for the simultaneous determination of sulphide and sulphite is described, which involves continuous H(2)S and SO(2) generation, preconcentration in a liquid nitrogen trap and measurement of the molecular absorption spectra of volatiles in the gas phase in 190-220 nm range. Under the recommended conditions (sample flow: 50 ml/min and concentrated sulphuric acid flow: 12 ml/min; generation time: 4 min) linear response ranges from 0.05 mug/ml for S(2-) and 0.20 mug/ml SO(2-)(3) are obtained with detection limits of 0.05 and 0.20 mug/ml respectively. Synthetic mixtures of the two components have been solved and a comparative study of different calculation methods has been made. In conclusion, multiwavelength methods offer better precision and accuracy.     

Spectrophotometric determination of paracetamol in drug formulations by oxidation with potassium dichromate

A rapid spectrophotometric method for determination of paracetamol is described, based on oxidation with dichromate for 15 min in 6M sulphuric acid at 80 degrees , and measurement (at 580 nm) of the chromium(III) formed. The method is applied to the determination of paracetamol in drugs prescribed for colds, coughs and flu. Of the common pharmaceuticals associated with paracetamol, only ascorbic acid and acetylsalicylic acid interfere. The results have been statistically compared with those obtained by the official (BP) and cerium(IV) methods.     

Anion-exchange separation and spectrophotometric determination of vanadium in silicate rocks

A combined anion-exchange-spectrophotometric method has been developed for the determination of vanadium in silicate rocks. A rock sample weighing about 0.1 g is decomposed with a mixture of sulphuric and hydrofluoric acids and after removal of HF the residue is taken up with dilute sulphuric acid. This solution is adjusted to be 0.05M in sulphuric acid and contain 0.3% hydrogen peroxide, and is passed through a column of Amberlite CG 400 (sulphate form). The sorbed vanadium is eluted with 30 ml of 1M hydrochloric acid. The effluent is evaporated to dryness, made 0.1M in hydrochloric acid and 3% in hydrogen peroxide content, and passed through a column of Amberlite CG 400 (chloride form) to get rid of accompanying thorium and zirconium. Vanadium is stripped by elution with 20 ml of 1M hydrochloric acid and subsequently determined spectrophotometrically with 4-(2-pyridylazo)resorcinol. The detection limit is 0.4 ppm.     

Simultaneous determination of vinburnine and 6-hydroxyvinburnine in human plasma by high-performance liquid chromatography

An isocratic high-performance liquid chromatographic method has been developed to allow the simple and rapid determination of both vinburnine (I) and its main metabolite, 6-hydroxyvinburnine (II), in heparinized human plasma (0.5 ml). Compounds I and II and p-chlorodisopyramide (internal standard) were first extracted with alkalinized ethyl acetate and then with sulphuric acid. Separation was achieved on a reversed-phase muBondapak C18 column with a mobile phase of acetonitrile-water-0.1 M heptanesulphonate in acetic acid and with detection at 254 nm. Each run required 20 min. The within-day coefficients of variation for identical samples (20 ng/ml) were 7 and 6% and between-day coefficients of variation 8 and 26% for I and II, respectively. The detection limit was 5 ng/ml (normal therapeutic concentration, 10-300 ng/ml). The application of the method to drug monitoring was compared to that of a thin-layer chromatographic procedure.     

Determination of thiamine using continuous flow molecular emission cavity analysis

A continuous flow method for the determination of thiamine hydrochloride (20.0-240.0 microgram ml(-1), 5.9 x 10(-5)-7.1 x 10(-4)m) is described. The sample was mixed with an excess of sodium hydroxide and remained in the delay coil for 20 min at 90 degrees C. The solution was then mixed with an excess of orthophosphoric acid and the hydrogen sulphide evolved was transferred continuously into the cavity to generate a molecular++ emission of S2. The analysis is completely automated, requires no sample pre-treatment and samples can be analysed at a rate of 30 samples h(-1) with a relative error of 1-2%. The method was evaluated by carrying out an interference study with common excipients and other water-soluble vitamins, a recovery study and by the analysis of commercial formulations. Results compared well with those obtained using the official method. The method was also applied to content uniformity tests.     

Flow injection analysis of sulphite by gas-phase molecular absorption UV/VIS spectrophotometry

A flow injection gas-phase molecular absorption spectrophotometric method is described for the determination of sulphite in aqueous solution. The sulphite solution, 200 microl, is introduced into a stream of distilled water. The carrier stream containing a sulphite zone is reacted, in the first mixing coil, with a stream of sulphuric acid (1 M). The evolved sulphur dioxide is purged to the segments of nitrogen flow through the second mixing coil. The gaseous phase is separated from the liquid stream by the use of a purpose built gas-liquid separator and then is swept into a purpose built flow-through cell. The absorbance of the gaseous phase is measured at 200 nm using a UV/VIS spectrophotometer. Up to 440 microg of sulphite is determined. The limit of detection is 0.8 microg and the R.D.S. for the determination of 70 and 220 microg of sulphite are 1.02 and 0.76%, respectively. Up to 40 samples h(-1) can be analyzed. The effect of several anions and cations on the determination of sulphite was studied and the results showed that the method is relatively free from interferences. The proposed method was applied to the determination of sulphite in a synthetic sample, water sample and lemon juice.     

Atomic fluorescence spectrometric determination of trace amounts of arsenic and antimony in drinking water by continuous hydride generation

A highly sensitive and simple method has been developed for the determination of As(III), total As, Sb(III) and total Sb in drinking water samples by continuous hydride generation and atomic fluorescence spectrometry (HGAFS). For As determination, water samples aspirated in a carrier of 2 mol l(-1) HCl were merged with a reducing NaBH(4) 3%(m/v) solution, with sample and NaBH(4) flow rates of 12.5 and 1.5 ml min(-1) respectively. The hydride generated in a 170 cm reaction coil was transported to the detector with an Ar flow of 400 ml min(-1), and a limit of detection between 5 and 20 ng l(-1) was obtained. For Sb determination, 2.5 mol l(-1) HCl and 2%(m/v) NaBH(4) were employed, with respective flow rates of 9.7 and 2 ml min(-1). The hydride generated in a 50 cm reaction coil was transported to the detector with an Ar flow rate of 300 ml min(-1), and a limit of detection between 6 and 14 ng l(-1) was obtained. Determination of the total concentration of these elements was obtained after a previous reduction with KI. Recovery studies of different added concentrations of these species in natural water samples were between 93 and 104% for As(III), 96-103% for As(V), 93-101% for Sb(III) and 90-119% for Sb(V).     

A rapid and mercury pollution-free redoximetry determination of total iron in copper ore

A rapid and mercury pollution-free method for the determination of total iron in the presence of copper is described. The sample was decomposed either by an acid attack of hydrochloric acid-nitric acid (1 + 2) or by fusion with sodium peroxide. The ferric ion in the sample solution was amenable to direct reduction to ferrous ion with potassium borohydride in sulphuric acid medium under the catalysis of cupric ion, followed by titration with potassium dichromate using sodium diphenylaminesulfonate as an indicator. After reduction, the iron (II) in the solution was stable for 300 min. The proposed method is free of interference from copper and has been successfully used for the large-scale routine determination of total iron in copper ores showing the same or better degree of precision and accuracy as those obtained by the classic standard stannous chloride-mercuric chloride method with the separation of iron from copper.     

Permanganate-based chemiluminescence analysis of cefadroxil monohydrate in pharmaceutical samples and biological fluids using flow injection

A chemiluminescent method using flow injection is described for the determination of cefadroxil monohydrate. The method is based on the chemiluminescence reaction of cefadroxil with potassium permanganate in sulphuric acid, sensitized by quinine. The proposed procedure allows the determination of cefadroxil over the concentration range 0.1-30 mug ml(-1) with a detection limit of 0.05 mug ml(-1) and a sample measurement frequency of 150 samples h(-1). The method was successfully applied to the determination of cefadroxil in pharmaceutical preparations and biological fluids.     

离子排斥色谱法测定生脉注射液中的有机酸

1引言生脉注射液是由红参、麦冬和五味子3种药材经提取后制成的灭菌水溶液,为国家中药保护品种,具有益气养阴,复脉固脱的功效。前期的分析实验表明,生脉注射液中含有有机酸类成分。根据生脉注射液的生产工艺和3种药材的的化学成分研究报道,分析生脉注射液中的有机酸主要来源于五味子。五味子含有柠檬酸、苹果酸、琥珀酸等多种有机酸成分。目前,有机酸的分析方法有气相色谱法[1]、高效液相色谱法[2]、毛细管电泳法[3]及离子色谱法[4]。这些方法专属[5]