Publication | Open Access
Selective Imaging of Active Pharmaceutical Ingredients in Powdered Blends with Common Excipients Utilizing Two-Photon Excited Ultraviolet-Fluorescence and Ultraviolet-Second Order Nonlinear Optical Imaging of Chiral Crystals
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Citations
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References
2012
Year
Pharmaceutical ScienceEngineeringChemistryOptical PropertiesChemical ImagePharmaceutical TechnologyApi DistributionAnalytical ChemistryBioimagingOptical SpectroscopyPhotophysical PropertyMolecular ImagingBiophysicsChiral CrystalsMedicineBiophotonicsPharmacologyOptical SensorsBiomolecular EngineeringOptical ImagingExcipientsBiomedical ImagingFluorescence MeasurementsSelective ImagingImagingActive Pharmaceutical IngredientsPharmaceutical ResearchDrug Analysis
Second order nonlinear optical imaging of chiral crystals (SONICC) and two-photon excited fluorescence measurements [both autofluorescence and two-photon excited UV-fluorescence (TPE-UVF)] were assessed for the selective detection of APIs relative to common pharmaceutical excipients. Active pharmaceutical ingredients (APIs) compose only a small percentage of most tabulated formulations, yet the API distribution within the tablet can affect drug release and tablet stability. Complementary measurements using either UV-SONICC (266 nm detection) or TPE-UVF were shown to generate signals >50-fold more intense for a model API (griseofulvin) than those produced by common pharmaceutical excipients. The combined product of the measurements produced signals >10(4)-fold greater than the excipients studied. UV-SONICC or TPE-UVF produced greater selectivity than analogous measurements with visible-light detection, attributed to the presence of aromatic moieties within the API exhibiting strong one and two photon absorption at ~266 nm. Complementary SONICC and fluorescence measurements allowed for the sensitive detection of the three-dimensional distribution of tadalafil within a Cialis tablet to a depth of >140 μm.
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