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首页> 外文期刊>Analytical methods >Fingerprinting of falsified artemisinin combination therapies via direct analysis in real time coupled to a compact single quadrupole mass spectrometer
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Fingerprinting of falsified artemisinin combination therapies via direct analysis in real time coupled to a compact single quadrupole mass spectrometer

机译:通过实时实时分析和紧凑型单四极杆质谱仪对伪造的青蒿素联合疗法进行指纹识别

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摘要

Falsified anti-malarial treatments continue to constitute a major health crisis, especially in malarious Africa. Even after detection of poor quality pharmaceuticals, it is critical that they be fully analyzed to determine their components, in order to assess their health effects and ultimately allow forensic tracing of their sources of production and distribution. Timely assessment requires robust and complete field-testing, or at the very least timely analysis after seizure or purchase. Ideally, low-cost and simple analytical equipment such as portable mass spectrometry (MS) is the best approach for achieving this quick and informative analysis. To date, Direct Analysis in Real Time (DART) MS has been successfully implemented to rapidly analyze falsified artemisinin-based combination therapies (ACTs) in laboratory settings, but this approach typically translates into high-cost and the need for high-resolution instrumentation. Here, we examine the use of DART ionization coupled with a portable low-resolution single-quadrupole instrument, and compare its success in fingerprinting anti-malarial tablets with higher resolution instrumentation. Using single quadrupole DART-MS, the same sample components were detected as with the high-resolution instrument, while needing significantly less consumables and power, and the additional advantages of increased portability and ease of use. Using Principal Component Analysis (PCA) of DART data, specific classes of falsified ACTs were identified, providing a more straightforward method for sourcing counterfeits and assessing their similarities.
机译:伪造的抗疟疾治疗继续构成重大的健康危机,尤其是在非洲疟疾流行的地区。即使在检测到劣质药物之后,也必须对它们进行全面分析以确定其成分,以评估其对健康的影响,并最终对他们的生产和分销来源进行法医追踪,这一点至关重要。及时评估需要强大而完整的现场测试,或者至少在扣押或购买后进行及时分析。理想情况下,低成本,简单的分析设备(例如便携式质谱仪(MS))是实现此快速,信息丰富的分析的最佳方法。迄今为止,已经成功实施了实时直接分析(DART)MS,可以在实验室环境中快速分析基于伪青蒿素的联合疗法(ACT),但是这种方法通常会导致高成本和高分辨率仪器的需求。在这里,我们研究了DART电离与便携式低分辨率单四极杆仪器结合使用的情况,并比较了其在高分辨率仪器上对抗疟疾药片进行指纹识别的成功率。使用单四极杆DART-MS,可以检测到与高分辨率仪器相同的样品成分,同时所需的消耗品和功率大大减少,并且具有增加的便携性和易用性的其他优点。使用DART数据的主成分分析(PCA),可以识别伪造的ACT的特定类别,从而提供了一种更直接的方法来寻找假冒产品并评估其相似性。

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