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硫酸奎纳普林载药油质纳米混悬剂在感染 T. evansi 的小鼠模型中的长期抗锥虫效果。

Long-term antitrypanosomal effect of quinapyramine sulphate-loaded oil-based nanosuspension in T. evansi-infected mouse model.

机构信息

Department of Pharmacy, Birla Institute of Technology and Science (BITS) Pilani, Pilani Campus, 333031, Pilani, Jhunjhunu, Rajasthan, India.

ICAR-National Research Centre on Camel, 334001, Jorbeer, Bikaner, Rajasthan, India.

出版信息

Drug Deliv Transl Res. 2024 Feb;14(2):542-554. doi: 10.1007/s13346-023-01419-3. Epub 2023 Aug 30.

DOI:10.1007/s13346-023-01419-3
PMID:37648938
Abstract

The goal of the present work consisted of the formulation development and evaluation of quinapyramine sulphate (QS)-loaded long-acting oil-based nanosuspension for improved antitrypanosomal effect. QS was transformed into a hydrophobic ionic complex using anionic sodium cholate (Na.C). The complex was characterized by FTIR, DSC, and XRD. Oil-based nanosuspension was prepared by dispersing the QS-Na.C complex in thixotropically thickened olive oil. The nanoformulation was found to be cytocompatible (82.5 ± 5.87% cell viability at the minimum effective concentration [MEC]) in THP-1 cell lines and selectively trypanotoxic (p < 0.0001). The pharmacokinetic studies of QS-Na.C complex-loaded oily nanosuspension showed 13.54-fold, 7.09-fold, 1.78-fold, and 17.35-fold increases in t, AUC, Vz/F, and MRT, respectively, as compared to free QS. Moreover, a 7.08-fold reduction in plasma clearance was observed after the treatment with the optimized formulation in Wistar rats. Furthermore, treatment with QS-Na.C complex-loaded oily nanosuspension (7.5 mg/kg) in T. evansi-infected mice model showed the absence of parasitaemia for more than 75 days after the treatment during in vivo efficacy studies. The efficacy of the treatment was assessed by observation of blood smear and PCR assay for DNA amplification. To conclude, our findings suggest that the efficient delivery of QS from the developed QS-Na.C complex-loaded oily nanosuspension could be a promising treatment option for veterinary infections against trypanosomiasis.

摘要

本工作的目的是开发和评价硫酸喹吡胺(QS)载长效油基纳米混悬剂,以提高抗锥虫作用。QS 被阴离子胆酸钠(Na.C)转化为疏水性离子配合物。该配合物通过傅里叶变换红外光谱(FTIR)、差示扫描量热法(DSC)和 X 射线衍射(XRD)进行了表征。油基纳米混悬剂是通过将 QS-Na.C 复合物分散在增稠的橄榄油中制备的。纳米制剂在 THP-1 细胞系中表现出细胞相容性(在最低有效浓度 [MEC] 时为 82.5 ± 5.87%细胞活力),并且具有选择性的杀锥虫作用(p < 0.0001)。QS-Na.C 复合物载油纳米混悬剂的药代动力学研究表明,与游离 QS 相比,t1/2、AUC、Vz/F 和 MRT 分别增加了 13.54 倍、7.09 倍、1.78 倍和 17.35 倍。此外,在 Wistar 大鼠中用优化制剂治疗后,观察到血浆清除率降低了 7.08 倍。此外,在 T. evansi 感染的小鼠模型中,用 QS-Na.C 复合物载油纳米混悬剂(7.5mg/kg)治疗后,在体内疗效研究中,治疗后超过 75 天未观察到寄生虫血症。通过观察血涂片和 DNA 扩增的 PCR 检测评估了治疗效果。总之,我们的研究结果表明,从开发的 QS-Na.C 复合物载油纳米混悬剂中有效递送 QS 可能成为兽医感染锥虫病的一种有前途的治疗选择。

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