In vitro evaluation of the synergistic antiviral effects of acemannan in combination with azidothymidine and acyclovir.

Molecular biotherapy Pub Date : 1991-12-01
J B Kahlon, M C Kemp, N Yawei, R H Carpenter, W M Shannon, B H McAnalley
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Abstract

The antiviral effects of selected combinations between acemannan (ACE-M), a long-chained, polydispersed, beta-(1,4)-acetylated mannan, were tested in combination with azidothymidine (AZT) and acyclovir (ACY) in vitro. The rationale for such combinations was based on the antiviral and immunomodulatory properties exhibited by ACE-M. In addition, the observed antiviral effects of ACE-M against human immunodeficiency virus type 1 (HIV-1) and other enveloped viruses appear to be related to modification of the glycosylation of viral glycoproteins. Therefore, the inhibitory effect of ACE-M does not overlap with that of AZT or ACY. The studies presented herein show that ACE-M combined with suboptimal noncytotoxic concentrations of AZT or ACY act synergistically to inhibit the replication of HIV-1 and herpes simplex virus type 1 (HSV-1), respectively. The median effect method was not applicable for analysis because the test compounds show mutually nonexclusive drug effects. For a meaningful evaluation and interpretation of the effects of drug combinations, the biological significance of combinations must be considered, that is, the protective effect of the combination, the noncytotoxicity of the combination, the mechanism(s) of action of the individual compounds comprising the combination, and so forth. With respect to effects on U1 cells latently infected with HIV-1, treatment with combinations of AZT and ACE-M does not potentiate virus replication.

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阿西甘露聚糖与叠氮多苷、阿昔洛韦联合应用的体外协同抗病毒效果评价。
研究了长链多分散β -(1,4)-乙酰化甘露聚糖(ACE-M)与azidothymidine (AZT)和acyclovir (ACY)联合使用的体外抗病毒效果。这种组合的基本原理是基于ACE-M所表现出的抗病毒和免疫调节特性。此外,观察到ACE-M对人类免疫缺陷病毒1型(HIV-1)和其他包膜病毒的抗病毒作用似乎与病毒糖蛋白的糖基化修饰有关。因此,ACE-M的抑制作用与AZT或ACY并不重叠。本文的研究表明,ACE-M与次优浓度的无细胞毒性AZT或ACY联合,分别协同抑制HIV-1和单纯疱疹病毒1型(HSV-1)的复制。中位效应法不适用于分析,因为测试化合物显示出相互非排他性的药物效应。为了对药物组合的效果进行有意义的评价和解释,必须考虑组合的生物学意义,即组合的保护作用,组合的非细胞毒性,组成组合的单个化合物的作用机制,等等。关于对潜伏感染HIV-1的U1细胞的影响,AZT和ACE-M联合治疗不会增强病毒复制。
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