Pharmaceutical Chemistry Department, Faculty of Pharmacy, Deraya University, New Minia, Egypt.
Pharmaceutical Chemistry Department, Faculty of Pharmacy, Deraya University, New Minia, Egypt.
Spectrochim Acta A Mol Biomol Spectrosc. 2021 Dec 5;262:120066. doi: 10.1016/j.saa.2021.120066. Epub 2021 Jun 10.
In this think about, assurance of lopinavir and ritonavir down to organic concentration level has been carried out. The assurance is based on expanding the selectivity of the spectrofluorimetric procedure by combining both subordinate and synchronous spectrofluorimetric approaches, which allow effective estimation of lopinavir at 248.8 nm and ritonavir at 300.1 nm within the nearness of each other at Δλ of 60 nm. Worldwide Conference on Harmonization approval rules were taken after to completely approve the strategy, and linearity was gotten for the two drugs over the extend of 0.4-2.4 µg mL for Lopinavir and 0.1-0.6 µg mL for ritonavir. Application of of the strategy was successfully carried out within the commercial tablets with great understanding with the comparison strategies. As the detection limits were down to 0.133 and 0.022 µg mL and quantitation limits were 0.395 and 0.068 µg mL for lopinavir and ritonavir, individually; the in vivo assurance of lopinavir and ritonavir in spiked plasma tests was pertinent. The rate recuperations in natural tests were 99.10 ± 0.77 and 99.54 ± 0.60 for lopinavir and ritonavir, individually. Water was utilized as the ideal weakening dissolvable within the proposed strategy which includes an eco-friendly justify.
在本次研究中,对洛匹那韦和利托那韦的浓度水平进行了保证。该保证基于通过结合从属和同步荧光分光光度法来扩展荧光分光光度法的选择性,这使得可以在 60nm 的 Δλ 附近有效地估计洛匹那韦在 248.8nm 和利托那韦在 300.1nm 的浓度。随后,采用了世界卫生组织协调会议批准规则来完全批准该策略,并且在 0.4-2.4μg/mL 范围内获得了两种药物的线性,对于洛匹那韦和利托那韦分别为 0.1-0.6μg/mL。该策略的应用在商业片剂中成功实施,并与比较策略进行了很好的比较。由于检测限分别降至 0.133 和 0.022μg/mL,定量限分别降至 0.395 和 0.068μg/mL,因此在血浆测试中对洛匹那韦和利托那韦进行了体内保证。在天然测试中,回收率分别为 99.10±0.77 和 99.54±0.60。水被用作该建议策略中的理想稀释溶剂,该策略具有环保的理由。
