首页> 美国卫生研究院文献>International Journal of Nanomedicine >Oral lipid-based nanoformulation of tafenoquine enhanced bioavailability and blood stage antimalarial efficacy and led to a reduction in human red blood cell loss in mice
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Oral lipid-based nanoformulation of tafenoquine enhanced bioavailability and blood stage antimalarial efficacy and led to a reduction in human red blood cell loss in mice

机译:基于口服脂质的他夫喹喹纳米制剂增强了生物利用度和血液阶段抗疟功效并导致小鼠人红细胞损失减少

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摘要

Tafenoquine (TQ), a new synthetic analog of primaquine, has relatively poor bioavailability and associated toxicity in glucose-6-phosphate dehydrogenase (G6PD)-deficient individuals. A microemulsion formulation of TQ (MTQ) with sizes <20 nm improved the solubility of TQ and enhanced the oral bioavailability from 55% to 99% in healthy mice (area under the curve 0 to infinity: 11,368±1,232 and 23,842±872 min·μmol/L) for reference TQ and MTQ, respectively. Average parasitemia in Plasmodium berghei-infected mice was four- to tenfold lower in the MTQ-treated group. In vitro antiplasmodial activities against chloroquine-sensitive and chloroquine-resistant strains of Plasmodium falciparum indicated no change in half maximal inhibitory concentration, suggesting that the microemulsion did not affect the inherent activity of TQ. In a humanized mouse model of G6PD deficiency, we observed reduction in toxicity of TQ as delivered by MTQ at low but efficacious concentrations of TQ. We hereby report an enhancement in the solubility, bioavailibility, and efficacy of TQ against blood stages of Plasmodium parasites without a corresponding increase in toxicity.
机译:Tafenoquine(TQ)是一种新的伯氨喹的合成类似物,在葡萄糖-6-磷酸脱氢酶(G6PD)缺乏的个体中具有相对较差的生物利用度和相关毒性。尺寸小于20 nm的TQ(MTQ)微乳液制剂可改善TQ的溶解度,并将健康小鼠的口服生物利用度从55%提高至99%(曲线0到无限远处的面积:11,368±1,232和23,842±872 min· (μmol/ L)分别作为参考TQ和MTQ。在MTQ治疗组中,伯氏疟原虫感染小鼠的平均寄生虫病率降低了四到十倍。对恶性疟原虫对氯喹敏感和耐氯喹的菌株的体外抗血浆活性表明最大抑菌浓度的一半没有变化,这表明微乳不影响TQ的固有活性。在G6PD缺乏症的人源化小鼠模型中,我们观察到在低但有效的TQ浓度下MTQ传递的TQ毒性降低。我们在此报告,TQ对疟原虫寄生虫血液阶段的溶解度,生物利用度和功效有所增强,而毒性没有相应增加。

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