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9-(4-羟基-3-羟甲基丁-1-基)鸟嘌呤(BRL 39123)在动物体内的抗疱疹病毒活性。

Antiherpesvirus activity of 9-(4-hydroxy-3-hydroxymethylbut-1-yl) guanine (BRL 39123) in animals.

作者信息

Boyd M R, Bacon T H, Sutton D

机构信息

Beecham Pharmaceuticals Research Division, Biosciences Research Centre, Great Burgh, Epsom, Surrey, England.

出版信息

Antimicrob Agents Chemother. 1988 Mar;32(3):358-63. doi: 10.1128/AAC.32.3.358.

Abstract

The antiviral activity of 9-(4-hydroxy-3-hydroxymethylbut-1-yl)guanine (BRL 39123) was assessed in several animal models of herpes simplex virus (HSV) infection. BRL 39123 was as active as acyclovir (ACV) when applied topically to guinea pigs with a cutaneous HSV type 1 (HSV-1) infection and was also active topically in an HSV-2 genital infection. Before systemic administration to infected animals, BRL 39123 and ACV were administered orally and subcutaneously to mice, and the blood was assayed for each compound by high-pressure liquid chromatography. When given systemically to mice infected cutaneously with HSV-1, BRL 39123 was as active as ACV. In mice infected intranasally with HSV-1 or HSV-2, single daily subcutaneous doses of BRL 39123 were more effective than equivalent treatment with ACV, reflecting the more persistent activity seen in cell culture and a more stable triphosphate within the infected cell. When the compounds were supplied in drinking water for this infection, BRL 39123 and ACV had similar potencies against HSV-1, although ACV was more active against an HSV-2 infection than BRL 39123 was. In mice infected intraperitoneally with HSV-1, BRL 39123 was 10-fold more potent than ACV and a single dose of BRL 39123 reduced virus replication within the peritoneal cavity more effectively than 3 doses of ACV given 1, 5, and 20 h after infection. Although BRL 39123 failed to eradicate the virus from mice latently infected with HSV-1, treatment initiated 5 h after infection of the ear pinna reduced the numbers of mice that developed latent infections.

摘要

在单纯疱疹病毒(HSV)感染的多种动物模型中评估了9-(4-羟基-3-羟甲基丁-1-基)鸟嘌呤(BRL 39123)的抗病毒活性。将BRL 39123局部应用于患有皮肤1型单纯疱疹病毒(HSV-1)感染的豚鼠时,其活性与阿昔洛韦(ACV)相当,在HSV-2生殖器感染中局部应用也具有活性。在对感染动物进行全身给药之前,将BRL 39123和ACV口服和皮下给予小鼠,并通过高压液相色谱法对每种化合物的血液进行检测。当对皮肤感染HSV-1的小鼠进行全身给药时,BRL 39123的活性与ACV相当。在经鼻感染HSV-1或HSV-2的小鼠中,每日单次皮下注射BRL 39123比等量的ACV治疗更有效,这反映了在细胞培养中观察到的更持久的活性以及感染细胞内更稳定的三磷酸酯。当通过饮用水供应这些化合物用于这种感染时,BRL 39123和ACV对HSV-1的效力相似,尽管ACV对HSV-2感染的活性比BRL 39123更强。在腹腔感染HSV-1的小鼠中,BRL 39123的效力比ACV高10倍,单剂量的BRL 39123比在感染后1、5和20小时给予的3剂量ACV更有效地减少了腹腔内的病毒复制。尽管BRL 39123未能从潜伏感染HSV-1的小鼠中根除病毒,但在耳廓感染后5小时开始治疗减少了发生潜伏感染的小鼠数量。

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