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检测与奥司他韦耐药相关的 H275Y 突变在严重大流行流感病毒 A/H1N1 09 感染中的快速出现。

Detection of the rapid emergence of the H275Y mutation associated with oseltamivir resistance in severe pandemic influenza virus A/H1N1 09 infections.

机构信息

Retroviral Genetics Laboratory, Center for Virus Research, Westmead Millennium Institute, Westmead, NSW 2145, Australia.

出版信息

Antiviral Res. 2010 Jul;87(1):16-21. doi: 10.1016/j.antiviral.2010.04.002. Epub 2010 Apr 10.

Abstract

In 2009 a new swine-origin influenza virus A/H1N1 (A/H1N1 09) emerged, causing the century's first pandemic. Most isolates of the new A/H1N1 09 virus are susceptible to neuraminidase inhibitors, but the H275Y mutation in the neuraminidase gene region associated with high-level oseltamivir resistance has been detected. Using rolling circle amplification (RCA) technology, 96 A/H1N1 09-specific RT-PCR positive clinical samples collected from 80 oseltamivir-treated and untreated patients were screened for the presence of the H275Y mutation. Samples positive for 275Y mutation by RCA were cloned and sequenced for confirmation. From 25 patients who had been treated with oseltamivir and remained A/H1N1 09 RT-PCR positive, we identified three (12%) individuals with the H275Y mutation: one immuno-suppressed adult, one immuno-competent adult and one child. Samples collected at multiple time points from the two adults showed a switch from wild-type oseltamivir-sensitive 275H to oseltamivir-resistant 275Y population after 9 days of treatment. The child had the 275Y mutation detected after being persistently A/H1N1 09 RT-PCR positive while receiving oseltamivir treatment. Resistance was not detected in 17 pre-treatment samples and 54 A/H1N1 09 RT-PCR positive outpatients. RCA demonstrates the rapid emergence of the H275Y resistance mutation in individuals with severe A/H1N1 09 infection receiving neuraminidase inhibitors. Rapid detection of oseltamivir resistance in severe infection is essential for patients to receive maximum therapeutic benefit. In the light of emerging resistance, close monitoring and understanding of the nature and dynamics of resistance mutations in newly emerging strains should be a priority.

摘要

2009 年出现了一种新型的猪源流感病毒 A/H1N1(A/H1N1 09),引发了本世纪的首次大流行。大多数新型 A/H1N1 09 病毒株对神经氨酸酶抑制剂敏感,但已检测到与高水平奥司他韦耐药相关的神经氨酸酶基因区域中的 H275Y 突变。使用滚环扩增(RCA)技术,对从 80 名接受奥司他韦治疗和未接受治疗的患者中采集的 96 份 A/H1N1 09 特异性 RT-PCR 阳性临床样本进行了筛查,以确定是否存在 H275Y 突变。通过 RCA 阳性的样本进行克隆和测序以确认。从 25 名接受奥司他韦治疗但 A/H1N1 09 RT-PCR 仍为阳性的患者中,我们鉴定出 3 名(12%)患者存在 H275Y 突变:1 名免疫抑制的成年人、1 名免疫功能正常的成年人和 1 名儿童。从两名成年人采集的多个时间点的样本显示,在接受奥司他韦治疗 9 天后,从野生型奥司他韦敏感的 275H 到奥司他韦耐药的 275Y 种群发生了转变。在接受奥司他韦治疗的过程中,该儿童的 A/H1N1 09 RT-PCR 持续呈阳性,检测到了 275Y 突变。在 17 份治疗前样本和 54 份 A/H1N1 09 RT-PCR 阳性门诊患者中未检测到耐药性。RCA 表明,在接受神经氨酸酶抑制剂治疗的严重 A/H1N1 09 感染患者中,H275Y 耐药突变迅速出现。快速检测严重感染中的奥司他韦耐药性对于患者获得最大治疗效果至关重要。鉴于出现耐药性,应优先密切监测和了解新出现的病毒株中耐药突变的性质和动态。

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