Abstract

BackgroundDespite its potential benefits over univariate, chemometrics is rarely utilized for optimizing sequential injection analysis (SIA) methods. Specifically, in previous vis-spectrophotometric SIA methods, chemometrically optimized conditions were confined within flow rate and reagent concentrations while other conditions were ignored.ResultsThe current manuscript reports, for the first time, a comprehensive screening of conditions controlling vis-spectrophotometric SIA. A new diclofenac assay method was adopted. The method was based on oxidizing diclofenac by permanganate (a major reagent) with sulfuric acid (a minor reagent). The reaction produced a spectrophotometrically detectable diclofenac form. The 26 full-factorial design was utilized to study the effect of volumes of reagents and sample, in addition to flow rate and concentrations of reagents. The main effects and all interaction order effects on method performance, i.e. namely sensitivity, rapidity and reagent consumption, were determined. The method was validated and applied to pharmaceutical formulations (tablets, injection and gel).ConclusionsDespite 64 experiments those conducted in the current study were cumbersome, the results obtained would reduce effort and time when developing similar SIA methods in the future. It is recommended to critically optimize effective and interacting conditions using other such optimization tools as fractional-factorial design, response surface and simplex, rather than full-factorial design that used at an initial optimization stage. In vis-spectrophotometric SIA methods those involve developing reactions with two reagents (major and minor), conditions affecting method performance are in the following order: sample volume > flow rate ≈ major reagent concentration >> major reagent volume ≈ minor reagent concentration >> minor reagent volume.

Highlights

  • Despite its potential benefits over univariate, chemometrics is rarely utilized for optimizing sequential injection analysis (SIA) methods

  • The British Pharmacopoeia (BP) recommends a classical potentiometric method for diclofenac assay in raw materials while a LC method is recommended for tablet and gel formulations [47]

  • The current work deals with the screening of conditions controlling spectrophotometric SIA and developing a new assay method for diclofenac

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Summary

Introduction

Despite its potential benefits over univariate, chemometrics is rarely utilized for optimizing sequential injection analysis (SIA) methods. In previous vis-spectrophotometric SIA methods, chemometrically optimized conditions were confined within flow rate and reagent concentrations while other conditions were ignored. Sequential injection analysis (SIA) is the second generation of an extended family called flow injection (FI) techniques [1]. SIA gathers valuable advantages, including automation, miniaturization, versatility and costeffectiveness, over other generations and versions of FI techniques. Recent articles reviewing the principles, developments and applications of FI techniques are available elsewhere [2,3]. On the other hand, optimizing experimental conditions is a prior in developing analytical methods. Since the introduction of SIA technique in 1990 [1], the survey has enumerated 639 articles.

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