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The helicase primase inhibitor, BAY 57-1293 shows potent therapeutic antiviral activity superior to famciclovir in BALB/c mice infected with herpes simplex virus type 1
被引:37
作者:
Biswas, Subhajit
Jennens, Lyn
Field, Hugh J.
机构:
[1] Univ Cambridge, Ctr Vet Sci, Sch Vet, Cambridge CB3 0ES, England
[2] Arrow Therapeut Ltd, London SE1 DB, England
关键词:
HSV;
helicase primase;
BAY;
57-1293;
famciclovir;
antiviral;
MURINE IMMUNOSUPPRESSION MODEL;
ANIMAL-MODELS;
DISEASE;
CHEMOTHERAPY;
VALACICLOVIR;
ACYCLOVIR;
RESISTANT;
HSV-1;
D O I:
10.1016/j.antiviral.2006.11.006
中图分类号:
R9 [药学];
学科分类号:
1007 ;
摘要:
BAY 57-1293 represents a new class of potent inhibitors of herpes simplex virus (HSV) that target the virus helicase primase complex. The present study was conducted using the zosteriform infection model in BALB/c mice. The helicase primase inhibitor, BAY 57-1293 was shown to be highly efficacious in this model. The beneficial effects of therapy were obtained rapidly (within 2 days) although the onset of treatment was delayed for I day after virus inoculation. The compound given orally, or intraperitoneally once per day at a dose of 15 mg/kg for 4 successive days was equally effective or superior to a much higher dose of famciclovir (1 mg/ml, i.e. approximately 140-200 mg/kg/day) given in the drinking water for 7 consecutive days, which, in our hands, is the most effective method for administering famciclovir to mice. In contrast to the vehicle-treated infected mice, all mice that received antiviral therapy looked normal and active with no mortality, no detectable loss of weight and no marked change in ear thickness. BAY 57-1293 and famciclovir reduced the virus titers in the skin to below the level of detection by days 3 and 7 post infection, respectively. In both BAY 57-1293 and famciclovir-treated mice, infectious virus titers in the ear pinna and brainstem remained below the level of detection. Consistent with these findings, BAY 57-1293 also showed a potent antiviral effect in an experiment involving a small number of severely immunocompromised athymic-nude BALB/c mice. (C) 2006 Elsevier B.V. All rights reserved.
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页码:30 / 35
页数:6
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