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十年登革热药物研发:进展与展望。

Ten years of dengue drug discovery: progress and prospects.

机构信息

Novartis Institute for Tropical Diseases, 10 Biopolis Road, 05-01 Chromos, Singapore 138670, Singapore.

出版信息

Antiviral Res. 2013 Nov;100(2):500-19. doi: 10.1016/j.antiviral.2013.09.013. Epub 2013 Sep 27.

DOI:10.1016/j.antiviral.2013.09.013
PMID:24076358
Abstract

To combat neglected diseases, the Novartis Institute of Tropical Diseases (NITD) was founded in 2002 through private-public funding from Novartis and the Singapore Economic Development Board. One of NITD's missions is to develop antivirals for dengue virus (DENV), the most prevalent mosquito-borne viral pathogen. Neither vaccine nor antiviral is currently available for DENV. Here we review the progress in dengue drug discovery made at NITD as well as the major discoveries made by academia and other companies. Four strategies have been pursued to identify inhibitors of DENV through targeting both viral and host proteins: (i) HTS (high-throughput screening) using virus replication assays; (ii) HTS using viral enzyme assays; (iii) structure-based in silico docking and rational design; (iv) repurposing hepatitis C virus inhibitors for DENV. Along the developmental process from hit finding to clinical candidate, many inhibitors did not advance beyond the stage of hit-to-lead optimization, due to their poor selectivity, physiochemical or pharmacokinetic properties. Only a few compounds showed efficacy in the AG129 DENV mouse model. Two nucleoside analogs, NITD-008 and Balapiravir, entered preclinical animal safety study and clinic trial, but both were terminated due to toxicity and lack of potency, respectively. Celgosivir, a host alpha-glucosidase inhibitor, is currently under clinical trial; its clinical efficacy remains to be determined. The knowledge accumulated during the past decade has provided a better rationale for ongoing dengue drug discovery. Though challenging, we are optimistic that this continuous, concerted effort will lead to an effective dengue therapy.

摘要

为了应对被忽视的疾病,诺华热带疾病研究所(NITD)于 2002 年由诺华公司和新加坡经济发展局共同出资成立。NITD 的使命之一是开发针对登革热病毒(DENV)的抗病毒药物,DENV 是最常见的蚊媒病毒病原体。目前,DENV 既没有疫苗,也没有抗病毒药物。本文回顾了 NITD 在登革热药物发现方面取得的进展,以及学术界和其他公司的主要发现。为了鉴定靶向病毒和宿主蛋白的 DENV 抑制剂,我们采用了四种策略:(i)使用病毒复制测定进行 HTS(高通量筛选);(ii)使用病毒酶测定进行 HTS;(iii)基于结构的计算机对接和合理设计;(iv)重新利用丙型肝炎病毒抑制剂用于 DENV。从发现靶点到临床候选药物的开发过程中,由于选择性差、物理化学或药代动力学性质不佳,许多抑制剂未能在从发现到先导化合物优化阶段取得进展。只有少数化合物在 AG129 DENV 小鼠模型中显示出疗效。两种核苷类似物,NITD-008 和 Balapiravir,进入了临床前动物安全性研究和临床试验,但都因毒性和效力不足而分别终止。宿主α-葡萄糖苷酶抑制剂 Celgosivir 目前正在进行临床试验;其临床疗效仍有待确定。过去十年积累的知识为正在进行的登革热药物发现提供了更好的依据。尽管具有挑战性,但我们乐观地认为,这种持续、协调的努力将带来有效的登革热疗法。

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