Failed Repurposing of Lysosomotropic Drugs for COVID-19 Treatment or Prevention

F. Marceau
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Abstract

The hope for the rapid discovery of an effective drug therapy for COVID-19 has led to several efforts to repurpose drugs approved for other indications. Lysosomotropic drugs, organic amines such as chloroquine, hydroxychloroquine, amiodarone and many others, were found to interfere with the viral life cycle in vitro but have failed in clinical trials. The properties of lysosomotropic drugs and the vacuolar cytopathology induced by them are briefly reviewed, including the critical role of lipophilicity, the central role of vacuolar (V)-ATPase for their concentration in acidic organelles, the altered function of these organelles including impaired endocytosis and secretion, macroautophagic accumulation and secondary phospholipidosis. The apparent preferential uptake of lysosomotropic drugs by phagocytic leukocytes (macrophages, neutrophils) and the high concentrations needed for a sustained disruption of vacuolar trafficking may have contributed to the failure of lysosomotropic drug repurposing for COVID-19.
在COVID-19治疗或预防中重新使用溶酶体药物失败
人们希望迅速发现一种有效的药物治疗COVID-19,这导致了几次努力,将批准用于其他适应症的药物重新用于其他用途。溶酶体药物,有机胺类药物,如氯喹、羟氯喹、胺碘酮等,在体外被发现会干扰病毒的生命周期,但在临床试验中失败了。本文综述了溶酶体药物的特性及其诱导的空泡细胞病理,包括亲脂性的关键作用,空泡(V)- atp酶在酸性细胞器中浓度的中心作用,这些细胞器的功能改变,包括内吞和分泌受损,巨噬性积累和继发性磷脂病。吞噬白细胞(巨噬细胞、中性粒细胞)明显优先摄取溶溶体药物,以及持续破坏液泡运输所需的高浓度,可能是导致溶溶体药物重新用于COVID-19失败的原因。
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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