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N-甲氧基碳胸腺嘧啶对小鼠正痘病毒感染的抗病毒活性及体内疗效的细胞系依赖性

Cell line dependency for antiviral activity and in vivo efficacy of N-methanocarbathymidine against orthopoxvirus infections in mice.

作者信息

Smee Donald F, Wandersee Miles K, Bailey Kevin W, Wong Min-Hui, Chu Chung K, Gadthula Srinivas, Sidwell Robert W

机构信息

Institute for Antiviral Research, Department of Animal, Dairy and Veterinary Sciences, Utah State University, Logan, UT 84322-5600, USA.

出版信息

Antiviral Res. 2007 Jan;73(1):69-77. doi: 10.1016/j.antiviral.2006.04.010. Epub 2006 May 5.

Abstract

A novel carbocyclic thymidine analog, N-methanocarbathymidine [(N)-MCT], was evaluated for inhibition of orthopoxvirus infections. Efficacy in vitro was assessed by plaque reduction assays against wild-type and cidofovir-resistant strains of cowpox and vaccinia viruses in nine different cell lines. Minimal differences were seen in antiviral activity against wild-type and cidofovir-resistant viruses. (N)-MCT's efficacy was affected by the cell line used for assay, with 50% poxvirus-inhibitory concentrations in cells as follows: mouse=0.6-2.2 microM, rabbit=52-90 microM, monkey=87 to >1000 microM, and human=39-220 microM. Limited studies performed with carbocyclic thymidine indicated a similar cell line dependency for antiviral activity. (N)-MCT did not inhibit actively dividing uninfected cells at 1000 microM. The potency of (N)-MCT against an S-variant thymidine kinase-deficient vaccinia virus was similar to that seen against S-variant and wild-type viruses in mouse, monkey, and human cells, implicating a cellular enzyme in the phosphorylation of the compound. Mice were intranasally infected with cowpox and vaccinia viruses followed 24h later by intraperitoneal treatment with (N)-MCT (twice a day for 7 days) or cidofovir (once a day for 2 days). (N)-MCT treatment at 100 and 30 mg/kg/day resulted in 90 and 20% survival from cowpox virus infection, respectively, compared to 0% survival in the placebo group. Statistically significant reductions in lung virus titers on day 5 occurred in 10, 30, and 100mg/kg/day treated mice. These same doses were also active against a lethal vaccinia virus (WR strain) challenge, and protection was seen down to 10mg/kg/day against a lethal vaccinia virus (IHD strain) infection. Cidofovir (100mg/kg/day) protected animals from death in all three infections.

摘要

一种新型碳环胸苷类似物,N-甲酰基碳环胸苷[(N)-MCT],被评估用于抑制正痘病毒感染。通过空斑减少试验评估其在九种不同细胞系中对野生型和西多福韦耐药的牛痘病毒和痘苗病毒株的体外疗效。在针对野生型和西多福韦耐药病毒的抗病毒活性方面观察到极小差异。(N)-MCT的疗效受用于试验的细胞系影响,在细胞中的50%痘病毒抑制浓度如下:小鼠=0.6 - 2.2微摩尔,兔=52 - 90微摩尔,猴=87至>1000微摩尔,人=39 - 220微摩尔。对碳环胸苷进行的有限研究表明抗病毒活性存在类似的细胞系依赖性。(N)-MCT在1000微摩尔时不抑制活跃分裂的未感染细胞。(N)-MCT对S变异型胸苷激酶缺陷痘苗病毒的效力与在小鼠、猴和人细胞中对S变异型和野生型病毒的效力相似,这表明一种细胞酶参与了该化合物的磷酸化。小鼠经鼻感染牛痘病毒和痘苗病毒,24小时后腹腔注射(N)-MCT(每天两次,共7天)或西多福韦(每天一次,共2天)进行治疗。与安慰剂组0%的存活率相比,(N)-MCT以100和30毫克/千克/天的剂量治疗分别使牛痘病毒感染的存活率达到90%和20%。在第5天,接受10、30和100毫克/千克/天治疗的小鼠肺病毒滴度有统计学显著降低。这些相同剂量对致死性痘苗病毒(WR株)攻击也有活性,并且在10毫克/千克/天的剂量下对致死性痘苗病毒(IHD株)感染有保护作用。西多福韦(100毫克/千克/天)在所有三种感染中均保护动物免于死亡。

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