Title of article :
Determination of active ingredients in cough–cold preparations by micellar liquid chromatography
Author/Authors :
Gil-Agust??، نويسنده , , Mayte and Monferrer-Pons، نويسنده , , Llorenç and Garc??a-Alvarez-Coque، نويسنده , , Mar??a Celia and Esteve-Romero، نويسنده , , Josep، نويسنده ,
Issue Information :
ماهنامه با شماره پیاپی سال 2001
Pages :
10
From page :
621
To page :
630
Abstract :
The chromatographic behaviour of some active ingredients in cough–cold pharmaceutical preparations, the antihistamine chlorpheniramine (or the dextro enantiomer dexchlorpheniramine), and the phenethylamines phenylephrine, phenylpropanolamine and pseudoephedrine, has been studied using a C18 column, micellar mobile phases of sodium dodecyl sulphate (SDS) and pentanol, and with UV detection. All possible combinations of chlorpheniramine/phenethylamine were resolved and determined using a mobile phase of 0.15 M SDS–6% (v/v) pentanol at pH 7, with analysis time below 7 min. Repeatabilities and within laboratory precisions were evaluated at four different drug concentrations in the range 0.5–25 μg ml−1 (n=5), resulting RSDs below 1.6%. The drug amounts found in the analysis of 14 commercialised preparations agreed with those declared by the manufacturers within the tolerance limits, and with those obtained using an aqueous 60% (v/v) methanol reference mobile phase. No interference was observed from other accompanying drugs such as acetylsalicylic acid, ascorbic acid, betamethasone, caffeine, codeine phosphate, diphenhydramine, lactose, paracetamol, and prednisolone. The studied combinations required a rather high amount of methanol in conventional RPLC to be eluted from the column. In contrast, the proposed procedure used a much lower amount of organic solvent (pentanol), which is highly retained in the SDS solution, being also less toxic than methanol.
Keywords :
Micellar liquid chromatography , Phenethylamines , Chlorpheniramine , Pharmaceuticals
Journal title :
Talanta
Serial Year :
2001
Journal title :
Talanta
Record number :
1641432
Link To Document :
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