In silico and in vitro screening of licensed antimalarial drugs for repurposing as inhibitors of hepatitis E virus.

In Silico Pharmacology Pub Date : 2021-05-04 eCollection Date: 2021-01-01 DOI:10.1007/s40203-021-00093-y

Borris Rosnay Tietcheu Galani, Vincent Brice Ayissi Owona, Romeo Joel Guemmogne Temdie, Karoline Metzger, Marie Atsama Amougou, Pascal Dieudonné Djamen Chuisseu, Arnaud Fondjo Kouam, Marceline Ngounoue Djuidje, Cécile-Marie Aliouat-Denis, Laurence Cocquerel, Paul Fewou Moundipa

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引用次数: 7

Abstract

Abstract: Hepatitis E virus (HEV) infection is emerging in Cameroon and represents one of the most common causes of acute hepatitis and jaundice. Moreover, earlier reports showed evidence of falciparum malaria/HEVcoexistence. Although the Sofosbuvir/Ribavirin combination was recently proposed in the treatment of HEV-infected patients, no specific antiviral drug has been approved so far, thereby urging the search for new therapies. Fortunately, drug repurposing offers a good alternative to this end. In this study, we report the in silico and in vitro activities of 8 licensed antimalarial drugs and two anti-hepatitis C virus agents used as references (Sofosbuvir, and Ribavirin), for repurposing as antiviral inhibitors against HEV. Compounds were docked against five HEV-specific targets including the Zinc-binding non-structural protein (6NU9), RNA-dependent RNA polymerase (RdRp), cryoEM structure of HEV VLP, genotype 1 (6LAT), capsid protein ORF-2, genotype 3 (2ZTN), and the E2s domain of genotype 1 (3GGQ) using the iGEMDOCK software and their pharmacokinetic profiles and toxicities were predicted using ADMETlab2.0. Their in vitro effects were also assessed on a gt 3 p6Gluc replicon system using the luciferase reporter assay. The docking results showed that Sofosbuvir had the best binding affinities with 6NU9 (- 98.22 kcal/mol), RdRp (- 113.86 kcal/mol), 2ZTN (- 106.96 kcal/mol), while Ribavirin better collided with 6LAT (- 99.33 kcal/mol). Interestingly, Lumefantrine showed the best affinity with 3GGQ (-106.05 kcal/mol). N-desethylamodiaquine and Amodiaquine presented higher binding scores with 6NU9 (- 93.5 and - 89.9 kcal/mol respectively vs - 80.83 kcal/mol), while Lumefantrine had the greatest energies with RdRp (- 102 vs - 84.58), and Pyrimethamine and N-desethylamodiaquine had stronger affinities with 2ZTN compared to Ribavirin (- 105.17 and - 102.65 kcal/mol vs - 96.04 kcal/mol). The biological screening demonstrated a significant (P < 0.001) antiviral effect on replication with 1 µM N-desethylamodiaquine, the major metabolite of Amodiaquine. However, Lumefantrine showed no effect at the tested concentrations (1, 5, and 10 µM). The biocomputational analysis of the pharmacokinetic profile of both drugs revealed a low permeability of Lumefantrine and a specific inactivation by CYP3A2 which might partly contribute to the short half-time of this drug. In conclusion, Amodiaquine and Lumefantrine may be good antimalarial drug candidates for repurposing against HEV. Further in vitro and in vivo experiments are necessary to validate these predictions.

Graphic abstract:

Supplementary information: The online version contains supplementary material available at 10.1007/s40203-021-00093-y.

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获得许可的抗疟疾药物作为戊型肝炎病毒抑制剂的体内和体外筛选

戊型肝炎病毒(HEV)感染正在喀麦隆出现，是急性肝炎和黄疸的最常见原因之一。此外，较早的报告显示了恶性疟疾/艾滋病毒共存的证据。尽管索非布韦/利巴韦林联合治疗最近被提议用于治疗hev感染患者，但迄今为止尚未批准特异性抗病毒药物，因此敦促寻找新的治疗方法。幸运的是，药物再利用为实现这一目标提供了一个很好的选择。在这项研究中，我们报告了8种获得许可的抗疟疾药物和两种作为参考的抗丙型肝炎病毒药物(索非布韦和利巴韦林)的体内和体外活性，以重新用作抗HEV的抗病毒抑制剂。使用iGEMDOCK软件将化合物对接到5个HEV特异性靶点，包括锌结合非结构蛋白(6NU9)、RNA依赖RNA聚合酶(RdRp)、HEV VLP的低温结构、基因1型(6LAT)、衣壳蛋白ORF-2、基因3型(2ZTN)和基因1型(3GGQ)的E2s结构域，并使用ADMETlab2.0预测它们的药代动力学特征和毒性。在g3p6gluc复制子系统上，使用荧光素酶报告基因法评估了它们的体外效应。对接结果表明，Sofosbuvir与6NU9 (- 98.22 kcal/mol)、RdRp (- 113.86 kcal/mol)、2ZTN (- 106.96 kcal/mol)的结合亲和力最好，而利巴韦林与6LAT (- 99.33 kcal/mol)的结合效果最好。有趣的是，发光芳碱与3GGQ的亲和力最好(-106.05 kcal/mol)。n -去乙基拉莫地喹和阿莫地喹与6NU9的结合分数较高(分别为- 93.5和- 89.9 kcal/mol，分别为- 80.83 kcal/mol)，鲁美曲明与RdRp的结合能量最高(分别为- 102和- 84.58)，乙胺嘧啶和n -去乙基拉莫地喹与2ZTN的亲和力较利巴韦林强(分别为- 105.17和- 102.65 kcal/mol，分别为- 96.04 kcal/mol)。图片摘要:补充资料:在线版本包含补充资料，可在10.1007/s40203-021-00093-y获得。

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In Silico Pharmacology

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