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首页> 外文期刊>Journal of Clinical Microbiology >Influenza Antiviral Resistance Testing in New York and Wisconsin, 2006 to 2008: Methodology and Surveillance Data
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Influenza Antiviral Resistance Testing in New York and Wisconsin, 2006 to 2008: Methodology and Surveillance Data

机译:2006年至2008年在纽约和威斯康星州进行的流感抗病毒耐药性检测:方法和监测数据

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The need for effective influenza antiviral susceptibility surveillance methods has increased due to the emergence of near-universal adamantane resistance in influenza A/H3N2 viruses during the 2005-2006 season and the appearance of oseltamivir resistance in the influenza A/H1N1 virus subtype during the 2007-2008 season. The two classes of influenza antivirals, the neuraminidase inhibitors (NAIs) and the adamantanes, are well characterized, as are many mutations that can confer resistance to these drugs. Adamantane resistance is imparted mainly by a S31N mutation in the matrix gene, while NAI resistance can result from a number of mutations in the neuraminidase gene. During the 2007-2008 season, a neuraminidase mutation (H274Y) conferring resistance to the NAI oseltamivir emerged worldwide in the A/H1N1 virus subtype. Surveillance methodology and data from New York (NY) and Wisconsin (WI) for the 2006-2007 and 2007-2008 influenza seasons are presented. We used an existing pyrosequencing method (R. A. Bright et al., Lancet 366:1175-1181, 2005) and a modified version of this method for detection of adamantane resistance mutations. For NAI resistance mutation detection, we used a mutation-specific pyrosequencing technique and developed a neuraminidase gene dideoxy sequencing method. Adamantane resistance in the A/H3N2 virus samples was 100% for 2007-2008, similar to the 99.8% resistance nationwide as reported by the CDC. Adamantane resistance was found in only 1.2% of NY and WI A/H1N1 virus samples, compared to that found in 10.8% of samples tested nationwide as reported by the CDC. Influenza A/H1N1 virus H274Y mutants were found in 11.1% of NY samples for 2007-2008, a level comparable to the 10.9% nationwide level reported by the CDC; in contrast, mutants were found in 17.4% of WI samples. These results indicate the need for regional influenza antiviral surveillance.
机译:由于在2005-2006赛季A / H3N2流感病毒中出现了近乎普遍的金刚烷耐药性,并且在2007年期间出现了A / H1N1流感病毒亚型中的奥司他韦耐药性,因此对有效的流感抗病毒敏感性监测方法的需求增加了-2008赛季。两种类型的流感抗病毒药,神经氨酸酶抑制剂(NAIs)和金刚烷类,已被很好地表征,许多突变都赋予了这些药物抗药性。金刚烷抗性主要由基质基因中的S31N突变赋予,而NAI抗性可由神经氨酸酶基因中的许多突变引起。在2007年至2008年季节期间,全世界范围内的A / H1N1病毒亚型均出现了赋予NAI奥司他韦耐药性的神经氨酸酶突变(H274Y)。介绍了2006-2007年和2007-2008年流感季节的纽约州(New York)和威斯康星州(wisconsin)(WI)的监视方法和数据。我们使用了现有的焦磷酸测序方法(R. A. Bright等人,《柳叶刀》 366:1175-1181,2005)和该方法的改进版本来检测金刚烷抗性突变。对于NAI抗性突变检测,我们使用了特定于突变的焦磷酸测序技术,并开发了一种神经氨酸酶基因双脱氧测序方法。 2007/2008年,A / H3N2病毒样品中的金刚烷抗药性为100%,类似于CDC报道的全国99.8%的抗药性。根据CDC的报告,在全国范围内测试的样本中,只有1.2%的NY和WI A / H1N1病毒样本发现了金刚烷抗药性。 2007年至2008年,在纽约州样本中发现了11.1%的A / H1N1流感病毒H274Y突变体,这一水平与美国疾病预防控制中心报告的全国10.9%的水平相当。相反,在WI样品中有17.4%发现了突变体。这些结果表明需要进行区域流感抗病毒监测。

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