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A Quinoline Compound Inhibits the Replication of Dengue virus Serotypes 1–4 in Vero Cells

登革热病毒 病毒学 维罗细胞 黄病毒 生物 登革热 血清型 喹啉 病毒复制 病毒 微生物学 化学 有机化学
作者
Hemalatha Beesetti,Poornima Tyagi,Brahmam Medapi,Vagolu Siva Krishna,Dharmarajan Sriram,Navin Khanna,S. Swaminathan
出处
期刊:Antiviral Therapy [SAGE Publishing]
卷期号:23 (5): 385-394 被引量:16
标识
DOI:10.3851/imp3231
摘要

Background The global occurrence of dengue, a mosquito-borne viral disease caused by four distinct dengue viruses (DENV-1, -2, -3 and -4), is reported to have increased approximately 30-fold in the last 50 years, causing approximately 400 million infections a year. A limited use, sub-optimal live attenuated dengue vaccine has become available recently. It is becoming apparent that antibodies to DENVs can promote infection by Zika virus (ZIKV), a related mosquito-borne flavivirus. A drug to treat these flaviviral infections continues to be an unmet public health need. Methods We screened an ‘in-house’ library of approximately 2,000 small molecules for inhibitors of cloned DENV-2 protease. Putative inhibitor binding to DENV-2 protease was analysed by in silico docking. Anti-DENV activity was analysed by monitoring viral antigen synthesis by ELISA, viral RNA synthesis by reverse-transcription coupled to real-time polymerase chain reaction and infectious virus production by plaque assay, in DENV-infected Vero cells. Results A quinoline derivative, BT24, was identified for the first time as a potent inhibitor of the cloned DENV-2 protease (half maximal inhibitory concentration [IC 50 ]=0.5 μM). In silico analysis revealed that BT24 binds to an allosteric site in the vicinity of the active site of DENV-2 protease. Cell-based assays demonstrated that BT24 can inhibit all four DENVs in infected Vero cells. Conclusions BT24 is a DENV-2 protease inhibitor which manifests the capacity to inhibit the replication of all four DENVs in cultured cells. It may provide a lead for a pan-DENV inhibitory drug.

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