Department of Chemistry, National Taiwan University, Taipei 106, Taiwan.
J Med Chem. 2012 Oct 11;55(19):8493-501. doi: 10.1021/jm3009844. Epub 2012 Sep 20.
Influenza therapy with a single targeted compound is often limited in efficacy due to the rapidly developed drug resistance. Moreover, the uncontrolled virus-induced cytokines could cause the high mortality of human infected by H5N1 avian influenza virus. In this study, we explored the novel dual-targeted bifunctional anti-influenza drugs formed by conjugation with anti-inflammatory agents. In particular, the caffeic acid (CA)-bearing zanamivir (ZA) conjugates ZA-7-CA (1) and ZA-7-CA-amide (7) showed simultaneous inhibition of influenza virus neuraminidase and suppression of pro-inflammatory cytokines. These ZA conjugates provided remarkable protection of cells and mice against influenza infections. Intranasal administration of low dosage (<1.2 μmol/kg/day) of ZA conjugates exhibited much greater effect than the combination therapy with ZA and the anti-inflammatory agents in protection of the lethally infected mice by H1N1 or H5N1 influenza viruses.
由于耐药性的迅速发展,单一靶向化合物治疗流感的疗效往往受到限制。此外,病毒诱导的细胞因子失控可能导致感染 H5N1 禽流感病毒的人类死亡率很高。在这项研究中,我们探索了通过与抗炎剂缀合形成的新型双重靶向双功能抗流感药物。特别是含有咖啡酸(CA)的扎那米韦(ZA)缀合物 ZA-7-CA(1)和 ZA-7-CA-酰胺(7)同时抑制流感病毒神经氨酸酶和抑制促炎细胞因子。这些 ZA 缀合物为细胞和小鼠提供了针对流感感染的显著保护。鼻内给予低剂量(<1.2 μmol/kg/天)的 ZA 缀合物的效果比扎那米韦和抗炎剂联合治疗对 H1N1 或 H5N1 流感病毒致死感染的小鼠的保护作用更大。
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