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[联合抗病毒药物体外作用的统计分析]

[Statistical analysis of the in-vitro action of combination antiviral agents].

作者信息

Sandow D, Hofmann F, Gröpler K, Nuhn P

机构信息

Institut für Medizinische Mikrobiologie, Bereiches Medizin Martin-Luther-Universität Halle-Wittenberg.

出版信息

Z Gesamte Hyg. 1990 Sep;36(9):471-4.

PMID:2173288
Abstract

Similar to the chemotherapy of bacterial infections, with the advanced development of virostatics a combination of antiviral agents is supposed to be introduced into the causal treatment of viral illness. The present studies explain a method for in vitro testing of virostatic combinations in cell cultures. The principle of the method is based on the checkerboard-technique used to test antibiotic combinations. As example the combination of trisodium phosphonoformate with bromovinyl-2'-deoxyuridine, acyclovir or 2-hexadecylglycero-3-phosphocholine was tested against herpes simplex virus, type 1. For evaluation of the test results the so-called reduction dose 50 (RD50) was introduced. The RD50 corresponds to this substance concentration, which reduces alone or in combination with a second virostatic the virus concentration used in the test system to its TCID50. With analogy to the calculation of infectious doses the computation of the RD50 was performed by using the method of Spearman and Kaerber. The calculated values allow the comparability of the antiviral activity of substances and their combinations. Corresponding to testing of antibiotics the further analysis of combinations was carried out by calculation of fractional inhibitory concentration (FIC), synergy factors (SF), and the construction of isobolograms. In this way, indifferent, synergistic and antagonistic effects of substance combination should be determined.

摘要

与细菌感染的化疗类似,随着抗病毒药物的不断发展,抗病毒药物联合使用有望应用于病毒疾病的病因治疗。目前的研究阐述了一种在细胞培养中体外测试抗病毒药物联合使用的方法。该方法的原理基于用于测试抗生素联合使用的棋盘技术。例如,以膦甲酸钠三钠与溴乙烯基-2'-脱氧尿苷、阿昔洛韦或2-十六烷基甘油-3-磷酸胆碱的联合使用为例,测试其对1型单纯疱疹病毒的效果。为了评估测试结果,引入了所谓的半数降低剂量(RD50)。RD50对应于这样一种物质浓度,该浓度单独或与另一种抗病毒药物联合使用时,可将测试系统中使用的病毒浓度降低至其半数组织培养感染剂量(TCID50)。与感染剂量的计算类似,RD50的计算采用Spearman和Kaerber方法。计算得到的值能够比较物质及其组合的抗病毒活性。与抗生素测试相对应,通过计算部分抑制浓度(FIC)、协同因子(SF)以及构建等效线图,对联合使用的药物进行进一步分析。通过这种方式,应确定物质组合的无关、协同和拮抗作用。

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