Searching for a long-acting injectable formulation for the antiretroviral dolutegravir

A. Marchi, C. Kobarg, Keity Margareth Doretto, Luis Gustavo Robello, M. Pigatto, M. Alves, R. Pereira
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引用次数: 1

Abstract

The aim of this study was to engineer a DTG particle size able to provide plasma drug concentration maintenance above PA-IC-90 and, based on such drug prolonged- exposure, to evaluate the 30 days-acting injectable DTG feasibility for anti-HIV therapy. Liquidantisolvent precipitation technology was used to engineer dolutegravir particles. As a strategy for controlling variations of the habit, particle size and polymorphs of Dolutegravir, process intensification was performed using acetone, methanol, and DMSO as solvents and a temperature range from 5oCto 30oC. Physical properties of particles were characterized and in vitro drug release was measured. As a pivotal characterization, in vivo pharmacokinetic analysis was conducted in Wistar male rats. Findings revealed that crystal habit and polymorph were solvent and temperature independents. Concerning solvents, particle sizes were not markedly different. However, results suggested that the higher the temperature the higher dolutegravir particle size. Particle size ranging from 6.48 µm to 17 µm (D50) shown an accelerated release rate and 93% of the drug were released up to 12th day. Results demonstrated thatDolutegravir particles of approximately 13 µm (D50) maintained plasma drug concentration above PA- IC90 for 26 days.
寻找抗逆转录病毒多替格拉韦的长效注射制剂
本研究的目的是设计一种DTG颗粒大小,能够使血浆药物浓度维持在PA-IC-90以上,并基于这种药物长时间暴露,评估30天可注射DTG抗hiv治疗的可行性。采用液相反溶剂沉淀法制备偏重颗粒。为了控制Dolutegravir的习性、粒径和多晶型的变化,采用丙酮、甲醇和DMSO作为溶剂,在50℃至30℃的温度范围内进行了工艺强化。对颗粒的物理性质进行了表征,并测定了其体外释放度。作为关键表征,在Wistar雄性大鼠体内进行了药代动力学分析。结果表明,晶体习性和晶型与溶剂和温度无关。溶剂的粒径差异不显著。然而,结果表明,温度越高,偏重粒子的粒径越大。粒径范围为6.48µm ~ 17µm (D50),释药速度加快,至第12天释药率为93%。结果表明,约13µm (D50)的多替替韦颗粒可使血浆药物浓度维持在PA- IC90以上26天。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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