首页> 外文期刊>Antiviral Research >Efficacy of therapeutic intervention with an oral ether-lipid analogue of cidofovir (CMX001) in a lethal mousepox model.
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Efficacy of therapeutic intervention with an oral ether-lipid analogue of cidofovir (CMX001) in a lethal mousepox model.

机译:用西多福韦的口服醚-脂质类似物(CMX001)在致死性老鼠痘模型中进行治疗干预的功效。

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摘要

In the 21st century we are faced with the potential use of natural or recombinant VARV and MPXV as biological weapons, and the emergence of human MPXV. Such an occurrences would require therapeutic and prophylactic intervention with antivirals. Cidofovir, an antiviral approved for the treatment of cytomegalovirus retinitis in AIDS patients, has activity against poxviruses, but must be administered intravenously and is associated with nephrotoxicity. An ether-lipid analogue of CDV, CMX001 (HDP-CDV), has potent antiviral activity against a range of DNA viruses including poxviruses, excellent oral bioavailability and minimal nephrotoxicity. CMX001 and CDV are equally efficacious at protecting mice from mortality following high ectromelia virus doses (10,000 x LD(50)) introduced by the intra-nasal route or small particle aerosol. Using CMX001 at a 10mg/kg dose followed by 2.5mg/kg doses every other-day for 14 days provided solid protection against mortality and weight loss following an intra-nasal challenge of (100-200) x LD(50) of ectromelia virus. Furthermore, complete protection against mortality was achieved when administration was delayed until as late as 5 days post-infection, which is 3-4 days prior to the death of the untreated controls. This therapeutic window would be equivalent to intervening during the rash stage of ordinary smallpox.
机译:在21世纪,我们面临着天然或重组天花病毒和MPXV作为生物武器的潜在使用,以及人类MPXV的出现。这种情况需要使用抗病毒药物进行治疗和预防干预。西多福韦(Cidofovir)是一种抗病毒药物,被批准用于治疗艾滋病患者的巨细胞病毒性视网膜炎,具有抗痘病毒的活性,但必须静脉注射并与肾毒性有关。 CDV的醚脂质类似物CMX001(HDP-CDV)对多种DNA病毒(包括痘病毒)具有有效的抗病毒活性,具有出色的口服生物利用度,且肾毒性最小。 CMX001和CDV同样有效地保护了小鼠免于因鼻内途径或小颗粒气雾剂引起的高剂量念珠菌病毒剂量(10,000 x LD(50))致死。鼻内攻击(100-200)x LD(50)的埃克森氏菌病毒后,以10mg / kg的剂量使用CMX001,然后每隔一天使用2.5mg / kg的剂量连续14天,可提供可靠的保护,防止死亡和体重减轻。此外,当给药延迟至感染后5天,即未治疗对照死亡前3-4天时,就获得了对死亡的完全保护。这种治疗窗口相当于在普通天花的皮疹阶段进行干预。

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