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Establishment of a Cell-Based Assay for Screening of Compounds Inhibiting Very Early Events in the Cytomegalovirus Replication Cycle and Characterization of a Compound Identified Using the Assay

机译:建立基于细胞的分析方法以筛选抑制巨细胞病毒复制周期中非常早期事件的化合物并鉴定使用该方法鉴定的化合物

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摘要

To simplify the detection of infectious human cytomegalovirus (HCMV), we generated a cell line that produced luciferase in a dose-dependent manner upon HCMV infection. Using this cell line, we identified anti-HCMV compounds from a diverse library of 9,600 compounds. One of them, 1-(3,5-dichloro-4-pyridyl)piperidine-4-carboxamide (DPPC), was effective against HCMV (Towne strain) infection of human lung fibroblast cells at a 50% effective concentration of 2.5 μM. DPPC also inhibited the growth of clinical HCMV isolates and guinea pig and mouse cytomegaloviruses. Experiments using various time frames for treatment of the cells with DPPC demonstrated that DPPC was effective during the first 24 h after HCMV infection. DPPC treatment decreased not only viral DNA replication but also IE1 and IE2 expression at mRNA and protein levels in the HCMV-infected cells. However, DPPC did not inhibit the attachment of HCMV particles to the cell surface. DPPC is a unique compound that targets the very early phase of cytomegalovirus infection, probably by disrupting a pathway that is important after viral entry but before immediate-early gene expression.
机译:为了简化感染性人类巨细胞病毒(HCMV)的检测,我们生成了一种细胞株,该细胞系在HCMV感染后以剂量依赖性方式产生萤光素酶。使用该细胞系,我们从9600种化合物的多样化文库中鉴定出抗HCMV化合物。其中一种是1-(3,5-二氯-4-吡啶基)哌啶-4-羧酰胺(DPPC),在50%有效浓度为2.5μM的情况下,可有效抵抗人肺成纤维细胞的HCMV(Towne株)感染。 DPPC还抑制临床HCMV分离株以及豚鼠和小鼠巨细胞病毒的生长。使用各种时间范围用DPPC处理细胞的实验表明,在HCMV感染后的最初24小时内,DPPC有效。 DPPC处理不仅降低了病毒DNA复制,而且还降低了HCMV感染细胞中mRNA和蛋白质水平的IE1和IE2表达。但是,DPPC不会抑制HCMV颗粒附着到细胞表面。 DPPC是针对巨细胞病毒感染早期阶段的独特化合物,可能通过破坏病毒进入后但立即早期基因表达之前重要的途径。

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