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在最近10株HSV-1临床分离株中的2株中,高频检测到对解旋酶-引发酶抑制剂BAY 57-1293高度耐药的HSV-1变异株。

Detection of HSV-1 variants highly resistant to the helicase-primase inhibitor BAY 57-1293 at high frequency in 2 of 10 recent clinical isolates of HSV-1.

作者信息

Biswas Subhajit, Smith Christopher, Field Hugh J

机构信息

Department of Veterinary Medicine, University of Cambridge, and Addenbrooke's Hospital, Cambridge CB3 0ES, UK.

出版信息

J Antimicrob Chemother. 2007 Aug;60(2):274-9. doi: 10.1093/jac/dkm182. Epub 2007 Jun 4.

DOI:10.1093/jac/dkm182
PMID:17550887
Abstract

OBJECTIVES

BAY 57-1293 is a helicase-primase inhibitor (HPI) from a new class of antivirals that are highly efficacious in herpes simplex virus (HSV)-1 animal infection models. Resistant mutants with point mutations in the helicase (UL5) were reported to be present in laboratory isolates at a low frequency of approximately 10(-6). In contrast, we have shown elsewhere that some laboratory isolates contain resistant variants at higher frequency (10(-4)). Therefore, we screened 10 recent clinical isolates of HSV-1 for BAY 57-1293-resistant virions.

METHODS

Clinical isolates were screened by a plaque reduction assay in Vero cells to determine the frequency of occurrence of BAY 57-1293-resistant variants. The helicase gene for the resistant variants was sequenced.

RESULTS

One isolate contained highly resistant variants at 10(-4) and another at 10(-5). Both variants contained a previously reported BAY 57-1293 resistance mutation (K356N) in UL5 and were >5000-fold resistant.

CONCLUSIONS

Occurrence of HPI-resistant viruses at high frequency in a clinical isolate is intriguing. Two alternative hypotheses are proposed to explain this phenomenon. It is also surprising that two unrelated clinical isolates contain an identical HPI resistance mutation. These results have important implications for HPI drug-resistance monitoring during subsequent clinical trials.

摘要

目的

BAY 57 - 1293是一种来自新型抗病毒药物的解旋酶 - 引发酶抑制剂(HPI),在单纯疱疹病毒(HSV)-1动物感染模型中具有高效性。据报道,在解旋酶(UL5)中存在点突变的耐药突变体在实验室分离株中以约10^(-6)的低频率出现。相比之下,我们在其他地方表明,一些实验室分离株含有更高频率(10^(-4))的耐药变体。因此,我们筛选了10株近期的HSV - 1临床分离株,以检测对BAY 57 - 1293耐药的病毒体。

方法

通过在Vero细胞中进行蚀斑减少试验来筛选临床分离株,以确定对BAY 57 - 1293耐药变体的出现频率。对耐药变体的解旋酶基因进行测序。

结果

一株分离株含有频率为10^(-4)的高耐药变体,另一株含有频率为10^(-5)的高耐药变体。这两种变体在UL5中均含有先前报道的BAY 57 - 1293耐药突变(K356N),且耐药性>5000倍。

结论

临床分离株中高频率出现HPI耐药病毒令人感兴趣。提出了两种替代假说来解释这一现象。同样令人惊讶的是,两株不相关的临床分离株含有相同的HPI耐药突变。这些结果对后续临床试验期间的HPI耐药性监测具有重要意义。

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