Broad-spectrum inhibitors targeting the viral replication promoter conserved in dengue and Zika viruses

针对登革热和寨卡病毒中保守的病毒复制启动子的广谱抑制剂

• 批准号: 10381583
• 负责人: Thomas C Hermann
• 金额: $ 19.35万
• 依托单位: UNIVERSITY OF CALIFORNIA, SAN DIEGO
• 依托单位国家: 美国
• 财政年份: 2021
• 资助国家: 美国
• 起止时间: 2021-04-01 至 2024-03-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/10381583
• 关键词: 3' Untranslated Regions; 5' Untranslated Regions; Address; Affect; Affinity; Antiviral Agents; Antiviral Therapy; Binding; Binding Sites; Biological Assay; Cell Culture Techniques; Cells; Central America; Clinical; Country; Dengue Fever; Dengue Hemorrhagic Fever; Dengue Virus; Development; Disease; Disease Outbreaks; Dose; Flavivirus; Fluorescence; Fluorescence Resonance Energy Transfer; Fluorescent Dyes; Future; Genome; Goals; Hepatitis C virus; Human; In Vitro; Label; Lead; Ligand Binding; Ligands; Liver Microsomes; Medical; Metabolic; Modeling; Molecular; Molecular Conformation; Monitor; Open Reading Frames; Outcome; Patients; Permeability; Polymerase; RNA; RNA Binding; RNA Conformation; RNA Sequences; RNA replication; RNA-Directed RNA Polymerase; Replication Initiation; Research; Risk; Sequence Alignment; Serotyping; Severities; Signal Transduction; South America; Structure; Symptoms; Testing; Therapeutic; Titrations; Toxic effect; Translations; Untranslated RNA; Vaccinee; Viral; Viral Genome; Virus Replication; ZIKV infection; Zika Virus; base; design; expression cloning; high throughput screening; inhibitor; inhibitor therapy; lead candidate; mosquito-borne; mosquito-borne pathogen; pandemic disease; pathogen; promoter; recruit; replicase; response; screening; small molecule; small molecule inhibitor; tissue culture; tool; viral RNA

Project Summary Zika virus (ZIKV) and dengue virus (DENV) are mosquito-borne flaviviruses that cause disease ranging in severity from mild symptoms to deadly hemorrhagic dengue fever. ZIKV was rapidly spreading five years ago to over 20 countries in South and Central America, where infections by ZIKV reached pandemic levels and threatened to expand to the southern US. The threat by DENV has increased dramatically over the last two decades as one of the worst mosquito-borne pathogens in tropical regions. To treat outbreaks of DENV in ZIKV-endemic regions, and vice versa, broad-spectrum inhibitor drugs against mosquito-borne flaviviruses would provide an efficient therapeutic approach that reduces the risk of immuno-associated exacerbation, for example in previously infected or vaccinated patients. Sequence alignment of DENV and ZIKV clinical isolates in combination with secondary structure prediction have led us to identify a conserved RNA three-way junction that serves as the replication promoter in flaviviruses. Here, we propose to identify compounds that inhibit viral replication by targeting the promoter RNA as lead candidates for the future development of DENV and ZIKV broad-spectrum therapeutics. The Specific Aims of this proposal are to 1) develop a FRET-based binding assay to assess small molecules as selective ligands of the DENV and ZIKV replication promoter RNA, 2) establish an in vitro replication initiation assay to identify promoter RNA-binding ligands as inhibitors of ZIKV replication, and 3) discover small molecules that inhibit DENV and ZIKV in cell culture by targeting the RNA 3WJ motif that serves as the viral replication promoter.

项目摘要 寨卡病毒（ZIKV）和登革热病毒（DENV）是蚊媒黄病毒，可引起多种疾病， 从轻微症状到致命的出血性登革热。ZIKV在五年前迅速蔓延 到南美洲和中美洲的20多个国家，ZIKV感染达到大流行水平， 威胁要扩张到美国南部。在过去两年中，DENV的威胁急剧增加， 几十年来，它一直是热带地区最严重的蚊媒病原体之一。治疗登革热的暴发， ZIKV流行地区，反之亦然，针对蚊媒黄病毒的广谱抑制剂药物 将提供一种有效的治疗方法，降低免疫相关恶化的风险， 例如，以前感染或接种疫苗的患者。 结合二级结构预测的DENV和ZIKV临床分离株的序列比对 已经使我们确定了一个保守的RNA三向连接，作为复制启动子， 黄病毒在这里，我们建议确定化合物，抑制病毒复制的目标启动子RNA 作为DENV和ZIKV广谱治疗剂未来发展的主要候选者。 本提案的具体目的是：1）开发基于FRET的结合试验，以评估小分子 作为DENV和ZIKV复制启动子RNA的选择性配体，2）建立体外复制 起始测定以鉴定启动子RNA结合配体作为ZIKV复制的抑制剂，和3）发现小的 通过靶向RNA 3WJ基序来抑制细胞培养物中的DENV和ZIKV的分子，所述RNA 3WJ基序充当病毒载体。 复制启动子