Ten years of dengue drug discovery: Progress and prospects

被引:278
|
作者
Lim, Siew Pheng [1 ]
Wang, Qing-Yin [1 ]
Noble, Christian G. [1 ]
Chen, Yen-Liang [1 ]
Dong, Hongping [1 ]
Zou, Bin [1 ]
Yokokawa, Fumiaki [1 ]
Nilar, Shahul [1 ]
Smith, Paul [1 ]
Beer, David [1 ]
Lescar, Julien [2 ]
Shi, Pei-Yong [1 ]
机构
[1] Novartis Inst Trop Dis, Singapore 138670, Singapore
[2] Nanyang Technol Univ, Sch Biol Sci, Singapore 637551, Singapore
关键词
Drug discovery; Antiviral; Dengue virus; Flavivirus; DEPENDENT RNA-POLYMERASE; VIRUS NS3 PROTEASE; SMALL-MOLECULE INHIBITORS; HEPATITIS-C; CRYSTAL-STRUCTURE; PEPTIDE INHIBITORS; CATALYTIC DOMAIN; IN-VITRO; HELICASE/NUCLEOSIDE TRIPHOSPHATASE; NONNUCLEOSIDE INHIBITORS;
D O I
10.1016/j.antiviral.2013.09.013
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
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. (C) 2013 Elsevier B.V. All rights reserved.
引用
收藏
页码:500 / 519
页数:20
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