| Literature DB >> 35658489 |
Hongxing Wang1,2,3, Yinzhou Fan1, Li Qin2, Zhipeng Cheng2, Xueqing Chen1, Sumei Zeng1, Shuanghong Liang1, Ying Tong2, Zhu Tao2, Yucheng Liu2, Xiaorong Liu4, Xiaohui Ning1, Peiquan Chen2, Siting Zhao2,5, Xiaoping Chen2,5.
Abstract
Liver-stage Plasmodium in humans is an early stage of malarial infection. Decoquinate (DQ) has a potent multistage antimalarial activity. However, it is practically water insoluble. In this study, the hot-melt extrusion (HME) approach was employed to prepare solid dispersions of DQ to improve oral bioavailability. The DQ dispersions were homogeneous in an aqueous suspension that contained most DQ (>90%) in the aqueous phase. Soluplus, a solubilizer, was found compatible with DQ in forming nanoparticle formulations during the HME process. Another excipient HPMC AS-126 was also proven to be suitable for making DQ nanoparticles through HME. Particle size and antimalarial activity of HME DQ suspensions remained almost unchanged after storage at 4°C for over a year. HME DQ was highly effective at inhibiting Plasmodium infection in vitro at both the liver stage and blood stage. HME DQ at 3 mg/kg by oral administration effectively prevented Plasmodium infection in mice inoculated with Plasmodium berghei sporozoites. Orally administered HME DQ at 2,000 mg/kg to mice showed no obvious adverse effects. HME DQ at 20 mg/kg orally administered to rats displayed characteristic distributions of DQ in the blood with most DQ in the blood cells, revealing the permeability of HME DQ into the cells in relation to its antimalarial activity. The DQ dispersions may be further developed as an oral formulation targeting Plasmodium infection at the liver stage.Entities:
Keywords: Plasmodium; Plasmodium infection; hot-melt extrusion; liver stage; nanoparticles; pharmaceutical formulation
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Year: 2022 PMID: 35658489 PMCID: PMC9211432 DOI: 10.1128/aac.02218-21
Source DB: PubMed Journal: Antimicrob Agents Chemother ISSN: 0066-4804 Impact factor: 5.938