4.6 Article

Chemometric quantitation of the active substance (containing CN) in a pharmaceutical tablet using near-infrared (NIR) transmittance and NIR FT-Raman spectra

期刊

APPLIED SPECTROSCOPY
卷 56, 期 5, 页码 579-585

出版社

SAGE PUBLICATIONS INC
DOI: 10.1366/0003702021955358

关键词

chemometrics; content uniformity; cyanide; iPLS; near-infrared transmittance; NIR; pharmaceutical; PLS; quantitative; Raman; tablets

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In this study, near-infrared (NIR) transmittance and Raman spectroscopy chemometric calibrations of the active substance content of a pharmaceutical tablet were developed using partial least-squares regression (PLS). Although the active substance contained the strongly Raman active Cequivalent toN functional group, the best results were obtained with NIR transmittance, which highlights the difference between (microscopic) surface sampling and whole tablet diffuse transmittance sampling. The tablets exist in four dosages with only two different concentrations of active substance (5 mg (5.6% w/w), and 10, 15, and 20 mg (8.0% w/w) active substance per tablet). A calibration on all four dosages resulted in a prediction error expressed as the root mean squared error of cross-validation (RMSECV) of 0.30% w/w for the NIR transmittance calibration. The corresponding error when using Raman spectra was 0-56% w/w. Specially prepared calibration batches covering the range 85-115% of the nominal content for each dosage were added to the first sample set, and NIR transmittance calibrations on this set-containing coated as well as uncoated tablets-gave a further reduction in prediction errors to 0.21-0.289% w/w. This corresponds to relative prediction errors (RMSECV/y(nom)) of 2.6-3.7%. This is a reasonable low error when compared to the error of the chromatographic reference method, which was estimated to 3.5%.

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