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Flow-injection spectrophotometric determination of captopril in pharmaceutical formulations using a new solid-phase reactor containing AgSCN immobilized in a polyurethane resin

Abstracts

A simple flow-injection analysis procedure was developed for determining captopril in pharmaceutical formulations employing a novel solid-phase reactor containing silver thiocyanate immobilized in a castor oil derivative polyurethane resin. The method was based on silver mercaptide formation between the captopril and Ag(I) in the solid-phase reactor. During such a reaction, the SCN- anion was released and reacted with Fe3+, which generated the FeSCN2+ complex that was continuously monitored at 480 nm. The analytical curve was linear in the captopril concentration range from 3.0 × 10-4 mol L-1 to 1.1 × 10-3 mol L-1 with a detection limit of 8.0 × 10-5 mol L-1. Recoveries between 97.5% and 103% and a relative standard deviation of 2% for a solution containing 6.0 × 10-4 mol L-1 captopril (n = 12) were obtained. The sample throughput was 40 h-1 and the results obtained for captopril in pharmaceutical formulations using this procedure and those obtained using a pharmacopoeia procedure were in agreement at a 95% confidence level.

AgSCN; Captopril; Flow-injection; Polyurethane resin; Solid-phase reactor


Um procedimento simples de análise por injeção em fluxo foi desenvolvido para a determinação de captopril em formulações farmacêuticas empregando um novo reator em fase sólida contendo tiocianato de prata imobilizado em resina poliuretana obtida a partir de óleo de mamona. O método foi baseado na formação de um mercapto composto de prata, no reator em fase sólida, obtido entre o captopril e Ag (I) imobilizada. Durante a reação, íons SCN- eram liberados e reagiam com Fe3+, gerando o complexo FeSCN2+, que foi continuamente monitorado em 480 nm. A curva analítica foi linear no intervalo de concentração de captopril entre 3,0 × 10-4 a 1,1 × 10-3 mol L-1 com um limite de detecção de 8,0 × 10-5 mol L-1. Recuperações entre 97,5-103% e desvio padrão relativo de 2% para uma solução contendo 6,0 × 10-4 mol L-1 de captopril (n = 12) foram obtidos. A frequência de amostragem foi de 40 h-1 e os resultados obtidos para captopril em formulações farmacêuticas utilizando este procedimento e o da Farmacopeia, estão de acordo em um nível de confiança de 95%.

AgSCN; Captopril; Injeção em fluxo; Resina poliuretana; Reator em fase sólida


ARTICLE

Flow-injection spectrophotometric determination of captopril in pharmaceutical formulations using a new solid-phase reactor containing AgSCN immobilized in a polyurethane resin

Fernando Campanhã VicentiniI; Willian Toito SuarezII; Éder Tadeu Gomes CavalheiroIII; Orlando Fatibello-FilhoI,* * Correspondence: O. Fatibello-Filho. Centro de Ciências Exatas e de Tecnologia, Departamento de Química, Universidade Federal de São Carlos. Rod. Washington Luis, km 235, Caixa Postal 676, 13.560-970 – São Carlos – SP, Brazil. E-mail: bello@ufscar.br

IDepartment of Chemistry, Federal University of São Carlos, UFSCar

IIDepartment of Chemistry, Federal University of Viçosa, UFV

IIIDepartment of Chemistry and Molecular Physics, University of São Paulo, USP

ABSTRACT

A simple flow-injection analysis procedure was developed for determining captopril in pharmaceutical formulations employing a novel solid-phase reactor containing silver thiocyanate immobilized in a castor oil derivative polyurethane resin. The method was based on silver mercaptide formation between the captopril and Ag(I) in the solid-phase reactor. During such a reaction, the SCN– anion was released and reacted with Fe3+, which generated the FeSCN2+ complex that was continuously monitored at 480 nm. The analytical curve was linear in the captopril concentration range from 3.0 × 10–4 mol L–1 to 1.1 × 10–3 mol L–1 with a detection limit of 8.0 × 10–5 mol L–1. Recoveries between 97.5% and 103% and a relative standard deviation of 2% for a solution containing 6.0 × 10–4 mol L–1 captopril (n = 12) were obtained. The sample throughput was 40 h–1 and the results obtained for captopril in pharmaceutical formulations using this procedure and those obtained using a pharmacopoeia procedure were in agreement at a 95% confidence level.

Uniterms: AgSCN. Captopril/determination. Flow-injection. Polyurethane resin. Solid-phase reactor.

RESUMO

Um procedimento simples de análise por injeção em fluxo foi desenvolvido para a determinação de captopril em formulações farmacêuticas empregando um novo reator em fase sólida contendo tiocianato de prata imobilizado em resina poliuretana obtida a partir de óleo de mamona. O método foi baseado na formação de um mercapto composto de prata, no reator em fase sólida, obtido entre o captopril e Ag (I) imobilizada. Durante a reação, íons SCN– eram liberados e reagiam com Fe3+, gerando o complexo FeSCN2+, que foi continuamente monitorado em 480 nm. A curva analítica foi linear no intervalo de concentração de captopril entre 3,0 × 10–4 a 1,1 × 10–3 mol L–1 com um limite de detecção de 8,0 × 10–5 mol L–1. Recuperações entre 97,5–103% e desvio padrão relativo de 2% para uma solução contendo 6,0 × 10–4 mol L–1 de captopril (n = 12) foram obtidos. A frequência de amostragem foi de 40 h–1 e os resultados obtidos para captopril em formulações farmacêuticas utilizando este procedimento e o da Farmacopeia, estão de acordo em um nível de confiança de 95%.

Unitermos: AgSCN. Captopril/determinação. Injeção em fluxo. Resina poliuretana. Reator em fase sólida.

INTRODUCTION

Captopril,1-[(2S)-3-mercapto-2-methyl propionyl]-l-proline (Figure 1) is an angiotensin converting enzyme (ACE) inhibitor, which reduces peripheral resistance and lowers blood pressure (Rubin et al., 1978). This compound can also be used to treat congestive heart failure (Goodman, Gilman, 1996). Captopril contains a sulphydryl group and forms disulphides and endogeneous thiol-containing compounds (cysteine, glutathione), as well as disulphide dimmer of the parent compound (Vancea et al., 2009).


Since it is widely used in high blood pressure control all over the world, numerous analytical methods have been developed for the quantitative determination of this analyte in pharmaceutical formulations. Methods based on titrimetric (Mohamed et al., 1983; Basavaiah, Prameela, 2004; Schmidt et al., 2009), spectrophotometric (Suarez et al., 2007; Suarez et al., 2009; Suarez et al., 2011), fluorimetric (Al-Ghannam et al., 2002; Chen, Cai, 2003), amperometric (Marcolino-Junior et al., 2009), conductometric (Lourenção et al., 2008), voltammetric (Ziyatdinova et al., 2006; Rezaei, Damiri, 2008; Karimi-Maleh et al., 2010), and chemiluminescence (Pulgarín et al., 2005) procedures have been previously described. The Brazilian Pharmacopeia recommends an iodimetric method for the determination of captopril in pharmaceutical formulations (Farmacopéia Brasileira, 1977).

The use of solid-phase reactors incorporated in flow-injection manifolds is a well-established methodology (Kojlo, Martínez-Calatayud, 1995). The reactor is generally constructed by incorporating oxidizing/reducing agents, insoluble salts, or ion exchange resins into a small column. The immobilization procedure is fairly expeditious, simple, and nonspecific (Pereira, Fatibello-Filho, 1998).

Solid-phase reactors are based on the immobilization of the reagents at a predefined point of the manifold. The sample zone is driven by the carrier stream through the reactor and conversion of the analyte takes place at the solid-solution interface (Tzanavaras, Themelis, 2007).

Some advantages of the use of solid-phase reactors in flow systems include lower consumption of reagents, greater stability, reproducible long-life supplies, and greater sensitivity and throughput.

Several procedures, utilizing solid-phase reactors that are based on the immobilization of insoluble salts such as Zn3(PO4)2 (Suarez et al., 2007), Ag2C6Cl2O4 (Suarez et al. 2009), Fe(OH)3 (Pereira, Fatibello-Filho, 1998), CoCO3 (Icardo et al., 1998; Corominas et al., 2005), AgCl (Marcolino-Junior et al., 2005), and PbO2 (Teixeira et al., 2002) in a polymeric matrix have been described in the literature. A typical immobilization procedure involves mixing the salt with polyester resin followed by the addition of a catalyst (methylethyl ketone).

Polyurethanes (PU) are versatile polymers that can be prepared as thermoplastic, thermosetting, elastomeric, foam, or adhesive by an appropriate choice of precursors. The remarkable properties of polyurethane include adhesion, abrasion electric resistance, hardness, chemical resistance to organic solvents, stability at low temperature, and tolerance to high humidity, as well as the ease of application, catalysis, and preparation of composite materials (Mendes et al., 2002). Another feature of the growing market demand is the use of polyols derived from vegetable oils (e.g. castor oil), a renewable source, and the simplicity of synthesis of derivatives, such as that used in the present study (Azevedo et al., 2009).

This study describes a new solid-phase reactor filled with an active phase consisting of silver thiocyanate dispersed in a castor oil polyurethane resin. The main advantages of such materials are their high resistance to organic solvents and the oily nature of the resin that provides a hydrophobic character to the final polymer, preventing a swelling effect from epoxy resins observed in other solid-phase reactors, when such materials are used in the aqueous media. Another interesting feature is that the polymer is composed from a bicomponent liquid system, the polyol (adhesive), and the prepolymer (hardener); the solid-phase is prepared by simply mixing the noncured precursors with the active reagent and the mixture is left to cure. The new reactor has been used in the determination of the antihypertensive captopril in pharmaceutical formulations, demonstrating its usefulness.

EXPERIMENTAL

Apparatus

The flow-injection system assembly is depicted in Figure 2. A peristaltic pump (Ismatec, model 7618-50, 8-channel, Zurich, Switzerland) supplied with Tygon® pump tubing was used for the propulsion of the solutions.


Sample and reference solutions were inserted into the flow system by a three-piece homemade manual injector-commutator made from Perspex containing two fixed bars and a sliding central bar (Krug et al., 1986).

Flow-injection spectrophotometric measurements were carried out using a Genesis 20 (Thermospectronics, USA) spectrophotometer, model 435, equipped with a homemade glass flow-cell (optical path, 1.0cm).

The molecular absorption spectra were obtained in a linear diode array Multispec 1501 spectrophotometer (Shimadzu, Japan), using a quartz cuvette with an optical path of 1.00 cm and volume of 4 mL.

Reagents and solutions

All solutions were prepared using water from an EasyPure RoDi purifying system (Barnstead, Thermo Scientific). All chemicals were analytical-reagent grade and were used without further purification.

The 5.0 × 10–3 mol L–1 captopril stock solution was prepared by dissolving 108.6 mg of this compound (Aldrich) in 1.0 × 10–2 mol L–1 HNO3 solution and completed in a 100.0 mL calibrated flask with the same acid solution. The reference solutions within the range of 3.0 × 10–4 mol L–1 to 1.1 × 10–3 mol L–1 were obtained by appropriate dilution of this stock solution with the same nitric acid solution in a 25.0 mL calibrated flask.

A 1.0 × 10–2 mol L–1 Fe(NO3)3.9H2O (Aldrich) solution was prepared by dissolving 404 mg in a 1.0 × 10–2 mol L–1 nitric acid solution, and the volume was made up to 100 mL in a calibrated flask using the same acid solution in order to prevent hydrolysis of the Fe(III) ion.

Preparation and analysis of the pharmaceutical samples

For analysis, Brazilian commercial tablets of captopril, containing 12.5 and 25.0 mg, according to the label, were used. Thus, 10 tablets of each formulation of the drug were weighed and powdered in a mortar. The resulting powder was diluted in deionized water and filtrated. Suitable dilutions were made to obtain a final concentration of captopril within the linear range of the analytical and analyzed curve using the developed flow procedure. The obtained results were compared with the standard iodime­tric procedure (Farmacopéia Brasileira, 1977).

Preparation and immobilization of AgSCN

For the preparation of the solid-phase reactor, 1.5 g AgSCN was mixed with 0.7 g of polyurethane resin and homogenized by manual mixing until an increase in the viscosity of the mixture was observed, and then kept at room temperature for 24 h. After this, it was ground in a Willy-type mill (Marconi, MA 048).

The particle size was selected by passing the pulverized material through stainless steel sieves (Bertel, Brazil) with different mesh sizes (35, 48, 60 and 100 mesh). The solid-phase reactor was constructed by packing particles of 60–100 mesh, which were inserted with the aid of a syringe, in PTFE tubing (100 mm long × 2.0 mm i.d). Pieces of glass wool were placed at both the ends of the tube to prevent fragment displacement through the transmission lines. The solid-phase reactor was inserted between the injector-commutator and the detector as shown in Figure 2.

RESULTS AND DISCUSSION

The principle of the determination of captopril employing a solid-phase reactor containing silver thiocyanate (AgSCN) is based on the following precipitation (1) and complex (2) reactions:

The reaction between silver thiocyanate and captopril leads to the displacement of thiocyanate and the formation of the well-known red complex with Fe(III) (Vogel, 1979; Baccan, 2001), which can be detected spectrophotometrically. When an aqueous captopril solution flowed through the solid-phase reactor packed with AgSCN entrapped in the polyurethane resin, SCN– ions were released from the reactor. The studies of chemical and hydrodynamic parameters were carried out using the flow-injection system depicted in Figure 2.

The univariated method was employed in all studies and was performed to identify a better balance between the magnitude and precision of analytical signals, the stability of baseline, and the sample throughput. The best conditions for the precipitation reaction between captopril and Ag (I) and the complex reaction between the anion thiocyanate displaced by the reactor and Fe (III) were studied.

Initially, the most appropriate carriers' solutions were tested, since the lifespan of the solid-phase reactor is directly related to the solution flowing through it. The acetate buffer was not studied once it forms a complex with Fe(III). In the same way, phosphate buffer was not used to prevent possible precipitation of FePO4(s). Sulfuric, hydrochloric, and phosphoric acids, as well as sodium and potassium hydroxides, were not tested since these acids and bases form insoluble salts with silver ions.

Thus, nitric acid solutions were studied as carriers. During this study, it was noted that the absorbance signals obtained using a 5.0 × 10–3 mol L–1 HNO3 solution were 20% lower than when using water. This decrease in the analytical signal is probably due to the difficulty in removing the acidic hydrogen from the captopril molecule (R-SH), because once in acidic medium, the displacement of the reaction toward the reactants occurs, as can be seen from the reaction represented in Eq. 1. Thus, water was employed in further experiments.

Reaction conditions and flow-injection parameters

The response of the flow-injection system was studied by varying the inner diameter and length of the reactor, the mass/mass ratios (AgSCN/polyurethane), and the particle sizes.

The internal diameter of the reactor was evaluated for 1.0, 1.5, 2.0, and 3.0 mm. The reactors with 1.0 and 1.5 mm were very difficult to pack. The reactor with 3.0 mm caused a pronounced dispersion of the sample zone. The reactor with 2.0 mm produced good sensitivity and adequate stability of the baseline and, consequently, was chosen for further experiments.

The influence of the solid-phase reactor length was evaluated from 3.0 to 12 cm. According to Figure 3, the absorbance signals increased with increments in the reactor length, but an undesirable increase of the hydrodynamic pressure was observed for reactors longer than 10.0 cm. So, a 10.0 cm reactor length was selected for further experiments.


The mass/mass ratios (AgSCN/polyurethane) of 1:2, 1:1, and 2:1 (m/m) were evaluated. The sensitivity (slope of the analytical curve) increased with the mass of AgSCN incorporated in the polyurethane resin, as shown in Figure 4. Thus, a 2:1 ratio was selected, taking into account the magnitude of the analytical signal.


The effect of particle size was studied in three size ranges (35–48, 48–60 and 60–100 mesh), selected by passing the particles through mesh sieves of known sizes. The 60–100 mesh particle size presented the highest absorbance signal and was selected for this reason.

Flow-injection parameters

The influence of Fe(III) concentration on the analytical signal was evaluated in the range from 3.0 × 10–3 to 5.0 × 10–2 mol L–1 for a 1.0 × 10–3 mol L–1 reference captopril solution. As can be seen in Figure 5, it was observed that the height of the peaks increased with the increase in Fe(III) concentration up to 1.0 × 10–2 mol L–1 and remained practically constant for higher concentrations of this reagent. Therefore, a 1.0 × 10–2 mol L–1 Fe(III) solution was chosen for further experiments.


Figure 6 shows the effect of the volumes of captopril inserted in the flow system by varying the volumes of the loop (L) between 100 and 700 µL, keeping the concentration of captopril at 1.0 × 10–3 mol L–1. The analytical signal increased from 100 to 500 µL for captopril, remaining almost constant at higher volumes. Consequently, the volume of 500 µL was chosen for the sample, based on the most effective balance of repeatability and magnitude of the analytical signal.


The influence of the reactor coil length (B) is shown in Figure 2, was also evaluated. The analytical signal was investigated in the 30–100 cm range. The analytical signal increased up to 50 cm, while higher lengths led to a decrease in the analytical signal because of sample dispersion. Consequently, a length of 50 cm for reactor coil B was selected.

The effect of the total flow rate was investigated in the range of 0.6–4.4 mL min–1. Best results were obtained with a flow rate of 1.1 mL min–1. For higher flow rates, the sensitivity decreased due to the short contact time between the sample zone and the silver thiocyanate particles in the solid-phase reactor. A flow rate of 1.1 mL min–1 was then selected taking into account the magnitude of the analytical signal, stability of the baseline, and low reagent consumption.

Table I presents the optimization of the chemical and flow-injection parameters studied in this work.

Analytical characteristics

Recoveries between 97.5% and 103% of captopril from five pharmaceutical formulations (n = 3) were obtained by using the flow-injection procedure. In this study, 2.0 × 10–1, 4.0 × 10–1 and 6.0 × 10–1 mmol L–1 of captopril were added to each product. The recovery results obtained suggest an absence of the matrix effect in the determination of captopril in those samples. Under optimum experimental conditions, the flow-injection system showed a linear response to captopril in the concentration range from 3.0 × 10–4 to 1.1 × 10–3 mol L–1 (A= 0.0714 + 281.25 C; r = 0.998, where A is the absorbance and C the concentration of captopril in mol L–1). The observed quantification limit (tenfold blank standard deviation/slope) was 1.0 × 10–4 mol L–1 and the detection limit (threefold blank standard deviation/slope) was 8.0 × 10–5 mol L–1. Typical transient signals corresponding to a linear calibration graph for captopril are shown in Figure 7.


The precision of the flow system was evaluated in two concentration levels (6.0 × 10–4 and 1.0 × 10-3 mol L-1). The relative standard deviations (RSDs) obtained were lower than 2% (n = 12) for both solutions and a sample throughput of 40 h–1 was attained. The transient signals are shown in Figure 8.


To examine the efficiency of the solid-phase reactor containing immobilized AgSCN in the polyurethane resin, experiments were performed with consecutive injections of captopril solutions. The reactors that were prepared presented high stability for at least eight hours under intense use in flowing solutions, when submitted to the consecutive injection of 3.0 × 10–4 to 1.1 × 10–3 mol L–1 captopril. After this period, a decrease in the order of 20% on the slope of the analytical curve was observed.

Determination of captopril in pharmaceutical formulations

The proposed flow-injection system was applied for the determination of captopril in pharmaceutical formulations. The results obtained by the proposed flow method and those obtained by the comparative method (Bittencount, 1977) are in agreement within a 95% confidence level (t-paired test), confirming the accuracy of the proposed flow-injection system employing a solid-phase reactor containing AgSCN immobilized in the polyurethane resin. The results of the analysis are given in Table II.

Table III shows the analytical characteristics obtained in this study and in other analytical systems developed for the determination of captopril. The primary advantage of the proposed flow-injection system is the lower generation of waste.

CONCLUSIONS

This study demonstrates the possibility of analyzing captopril in pharmaceutical products using a flow-injection system with spectrophotometric detection and could be extended to determine other drugs since it generates a precipitate with silver ions. The proposed method is simple, quick, and could be carried out with good precision and accuracy. The new solid-phase reactor containing AgSCN immobilized in the developed polyurethane resin derived from vegetable oil is easy to make and has a long lifetime of 500 reproducible results. As the polyurethane resin used here is an inert material with mechanical resistance it proved to be an interesting material for the preparation of solid reactors containing modifiers.

ACKNOWLEDGMENTS

The authors gratefully acknowledge the financial support provided by Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq), Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES), and Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP).

Received for publication on 21st December 2011

Accepted for publication on 10th May 2012

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  • *
    Correspondence: O. Fatibello-Filho. Centro de Ciências Exatas e de Tecnologia, Departamento de Química, Universidade Federal de São Carlos. Rod. Washington Luis, km 235, Caixa Postal 676, 13.560-970 – São Carlos – SP, Brazil. E-mail:
  • Publication Dates

    • Publication in this collection
      18 July 2012
    • Date of issue
      June 2012

    History

    • Received
      21 Dec 2011
    • Accepted
      May 2012
    Universidade de São Paulo, Faculdade de Ciências Farmacêuticas Av. Prof. Lineu Prestes, n. 580, 05508-000 S. Paulo/SP Brasil, Tel.: (55 11) 3091-3824 - São Paulo - SP - Brazil
    E-mail: bjps@usp.br