Cannalire Rolando, Ki Chan Kitti Wing, Burali Maria Sole, Gwee Chin Piaw, Wang Sai, Astolfi Andrea, Massari Serena, Sabatini Stefano, Tabarrini Oriana, Mastrangelo Eloise, Barreca Maria Letizia, Cecchetti Violetta, Vasudevan Subhash G, Manfroni Giuseppe
Dipartimento di Scienze Farmaceutiche, Università degli Studi di Perugia, Via del Liceo, 1-06123 Perugia, Italy.
Program in Emerging Infectious Diseases, Duke-NUS Medical School, 8 College Road, Singapore 169857.
ACS Med Chem Lett. 2020 Mar 19;11(5):773-782. doi: 10.1021/acsmedchemlett.9b00619. eCollection 2020 May 14.
Treatment of dengue virus (DENV) and other flavivirus infections is an unmet medical need. The highly conserved flaviviral NS5 RNA-dependent RNA polymerase (RdRp) is an attractive antiviral target that interacts with NS3 and viral RNA within the replication complex assembly. Biochemical and cell-based evidence indicate that targeting cavity B may lead to dual RdRp and NS5-NS3 interaction inhibitors. By ligand-based design around 1-pyrido[2,1-][1,3]benzothiazol-1-one (PBTZ) , we identified new potent and selective DENV inhibitors that exert dual inhibition of NS5 RdRp and NS3-NS5 interaction, likely through binding cavity B. Resistance studies with compound generated sequence variants in the 3'-untranslated region of RNA while further biochemical experiments demonstrated its ability to block also RNA-NS5 interaction, required for correct RNA synthesis in cells. These findings shed light on the potential mechanism of action for this class of compounds, underlying how PBTZs are very promising lead candidates for further evaluation.
登革热病毒(DENV)及其他黄病毒感染的治疗是一项尚未满足的医疗需求。高度保守的黄病毒NS5 RNA依赖性RNA聚合酶(RdRp)是一个有吸引力的抗病毒靶点,它在复制复合体组装过程中与NS3和病毒RNA相互作用。生化和细胞实验证据表明,靶向B腔可能会产生RdRp和NS5-NS3相互作用的双重抑制剂。通过围绕1-吡啶并[2,1-][1,3]苯并噻唑-1-酮(PBTZ)进行基于配体的设计,我们鉴定出了新的强效且选择性的DENV抑制剂,这些抑制剂可能通过结合B腔对NS5 RdRp和NS3-NS5相互作用发挥双重抑制作用。对化合物进行的耐药性研究在RNA的3'非翻译区产生了序列变异,而进一步的生化实验表明它还能够阻断细胞中正确RNA合成所需的RNA-NS5相互作用。这些发现揭示了这类化合物的潜在作用机制,即PBTZ为何是非常有前景的进一步评估先导候选物的基础。
