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Comparative Evaluation of Virus Transmission Inhibition by Dual-Acting Pyrimidinedione Microbicides Using the Microbicide Transmission and Sterilization Assay

机译:使用杀微生物剂传播和灭菌方法对双效嘧啶二酮杀微生物剂对病毒传播抑制的比较评估

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摘要

In the absence of a fully effective human immunodeficiency virus (HIV) vaccine, topical microbicides represent an important strategy for preventing the transmission of HIV through sexual intercourse, the predominant mode of HIV transmission worldwide. Although a comprehensive understanding of HIV transmission has not yet emerged in the microbicide field, it is likely the result of rapid infection of monocyte-derived cells in the vaginal mucosa by CCR5-tropic viruses. Inhibition of HIV transmission requires agents that prevent entry, fusion, reverse transcription, or other preintegrative replication events or agents which directly inactivate HIV or modulate the target cells to render them uninfectible. In vitro assays typically used to evaluate the ability of a microbicide to prevent virus transmission use epithelial or human osteosarcoma-derived cells or immune cells more relevant to the development of anti-HIV therapeutic agents and quantify virus production at short time intervals following infection. We have developed a microbicide transmission and sterilization assay (MTSA) to more sensitively and quantitatively evaluate virus transmission in cell culture in the presence of microbicidal compounds. Results obtained with the MTSA demonstrate that the inhibitory capacity of microbicides is often overestimated in short-term transmission inhibition assays, while some compounds yield equivalent inhibitory results, indicating a biological relevance for the MTSA-based evaluations to identify superior potent microbicides. The MTSA defines the concentration of the microbicide required to totally suppress the transmission of virus in cell culture and may thus help define the effective concentration of the microbicide required in a formulated microbicide product.
机译:在没有完全有效的人类免疫缺陷病毒(HIV)疫苗的情况下,局部杀微生物剂是防止HIV通过性交传播的重要策略,而性交是全世界HIV传播的主要方式。尽管在杀微生物剂领域还没有对HIV传播的全面了解,但这很可能是CCR5嗜性病毒迅速感染阴道粘膜中单核细胞衍生细胞的结果。抑制HIV传播需要防止进入,融合,逆转录或其他整合前复制事件的药物,或直接使HIV灭活或调节靶细胞使其不可感染的药物。通常用于评估杀微生物剂防止病毒传播的能力的体外分析方法是使用与抗HIV治疗剂的开发更相关的上皮细胞或人骨肉瘤衍生的细胞或免疫细胞,并在感染后的短时间内量化病毒的产生。我们已经开发了杀微生物剂传播和灭菌测定(MTSA),以在存在杀微生物化合物的情况下更敏感和定量地评估细胞培养中的病毒传播。用MTSA获得的结果表明,在短期传播抑制试验中,杀菌剂的抑制能力常常被高估,而某些化合物产生的抑制效果相当,这表明基于MTSA的鉴定潜在有效杀菌剂的评估具有生物学意义。 MTSA定义了完全抑制病毒在细胞培养中传播所需的杀微生物剂浓度,因此可以帮助确定配制的杀微生物剂产品中所需的杀微生物剂有效浓度。

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