ABSTRACT
Two chemists employed a three-device rapid screening "toolkit" consisting of a handheld Raman spectrometer, transportable mass spectrometer, and portable Fourier transform infrared (FT-IR) spectrometer at an international mail facility (IMF) satellite laboratory to examine unknown (unlabeled/mislabeled) products for the presence of active pharmaceutical ingredients (APIs). Phase I of this project previously demonstrated that this toolkit was the most effective collection of instruments for identifying APIs in product types collected at IMFs during a nationwide mail blitz and Phase II of this project previously demonstrated that results generated using the toolkit during a satellite laboratory pilot program were as reliable as those generated by a full-service library when two or more of these instruments identify an API. This study (Phase III) described the results of the satellite laboratory toolkit during production mode and encompassed the period ranging from June 2021 through December 2022. During this study, a total of 858 products were examined on-site at the IMF. The satellite laboratory yielded conclusive results for 726 (84.6%) products, which were used to support regulatory action, and identified 132 (15.4%) products that required additional full-service laboratory analyses due to inconclusive results. The satellite and full-service laboratory verified/confirmed at least one API/related substance in 617 (71.9%) products. A total of 709 APIs/related substances were found in the 617 products, and 202 of these 709 compounds were unique/different. Overall, during Phases I through III of this program, 350 different substances have been identified in products collected at IMFs.
Subject(s)
Mass Spectrometry , Humans , Pharmaceutical Preparations/analysis , Mass Spectrometry/methods , Spectroscopy, Fourier Transform Infrared , Spectrum Analysis, Raman , Drug Labeling , Postal Service , Laboratories , Bulk DrugsABSTRACT
A satellite laboratory "toolkit" consisting of a handheld Raman spectrometer, portable direct analysis in real-time mass spectrometer (DART-MS) and portable Fourier transform infrared (FT-IR) spectrometer was employed to examine 926 pharmaceutical, unknown and dietary supplement products collected at an international mail facility (IMF) for the presence of declared and undeclared active pharmaceutical ingredients (APIs) over the course of 68 working days. The toolkit successfully identified over 650 APIs, including over 200 unique APIs, using two or more devices. The performance of each individual device, and toolkit as a whole, were evaluated on all products and a subset of the products was forwarded to full-service laboratories for confirmatory analysis to determine false positive and false negative rates of the toolkit. The subset consisted of seven negative items (those not found to contain APIs using the toolkit) and 124 positive items (those found to contain at least one API using the toolkit). Overall, no false positives were detected in the negative items and only four false negatives and five false positives were detected in the positive items. Regarding the positive items, 119 of the 124 items were found to contain at least one API using at least two toolkit devices; each of these APIs were confirmed by a full-service laboratory. Furthermore, 90.2% of the APIs found by confirmatory laboratory analysis were detected by at least two toolkit devices. Based on these metrics and the fact that no false positives were detected by more than one device, it was concluded that when the toolkit detects and subsequently verifies/confirms an API using two or more devices, the results are as reliable as those generated by a full-service laboratory.
Subject(s)
Laboratories , Postal Service , Fourier Analysis , Spectroscopy, Fourier Transform Infrared , Pharmaceutical PreparationsABSTRACT
BACKGROUND: E-cigarette, or vaping, product use-associated lung injury was reported in over 2800 cases from August 2019 to February 2020. Samples of vaping products were submitted for laboratory analysis in conjunction with investigation of the outbreak. A rapid screening method that was selective and sensitive for multiple analytes was required to aid in the investigation. OBJECTIVE: To develop a multi-analyte method capable of screening vaping liquid samples that consumed small amounts of sample, required minimal sample preparation and analysis time, employed automated data processing, and provided the necessary sensitivity and selectivity. METHODS: Vaping liquids were dissolved in acetonitrile and sampled with DIP-it® tips. The tips were analyzed by direct analysis in real-time mass spectrometry (DART-MS) and the resulting data processed with TraceFinder™ software. Laboratory-fortified samples consisting of various analytes and matrixes were evaluated prior to the analysis of submitted samples. RESULTS: The method was successful at detecting all target analytes in all matrixes evaluated, although the method detection limits varied by analyte/matrix combination: from 0.1% nicotine in poly(propylene glycol) average Mn 1000 (the lowest level evaluated) to 5.0% poly(ethylene glycol) average Mn 400 in cannabis concentrate. Results for the analysis of submitted samples by this method compared favorably to GC-MS and FTIR results. CONCLUSION: The DART-MS method met the objective of speed, sensitivity, and selectivity (although certain cannabinoid isomers could not be distinguished). The method may be easily adapted or expanded for additional analytes. HIGHLIGHTS: This is a simple DART-MS method for screening vaping liquids for substances of concern in less than 2 min per sample.
Subject(s)
Cannabis , Electronic Nicotine Delivery Systems , Vaping , Mass Spectrometry/methods , Gas Chromatography-Mass SpectrometryABSTRACT
A "toolkit" consisting of a handheld Raman spectrometer equipped with a 1064 nm laser, a portable Fourier transform infrared (FT-IR) spectrometer and a portable direct analysis in real-time mass spectrometer (DART-MS) was employed in a laboratory setting to examine 82 representative products collected during a nationwide mail blitz for the presence of APIs. These results were compared to those obtained using laboratory-based methods; 8 of the products were not found to contain APIs and 74 of the products were found to contain a total of 88 APIs (65 of the 88 APIs were unique). The individual performance of each device and combined performance of the three-device toolkit were evaluated with regard to true positives, true negatives, false positives and false negatives. Using this toolkit, 81 (92.0 %) of the APIs were detected by at least one technique and 47 (64.8 %) of the APIs were detected by at least two techniques. Seven false negatives (8.0 %) were encountered and while the toolkit yielded 12 false positives, no false positives were detected by more than one technique. Overall, this study demonstrated that when the toolkit detects an API using two or more devices, the results are as reliable as those generated by a full-service laboratory.
