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美国从人分离的猪源流感病毒的抗病毒敏感性。

Antiviral Susceptibility of Swine-Origin Influenza A Viruses Isolated from Humans, United States.

出版信息

Emerg Infect Dis. 2024 Nov;30(11):2303-2312. doi: 10.3201/eid3011.240892. Epub 2024 Oct 8.

DOI:10.3201/eid3011.240892
PMID:39378870
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11521183/
Abstract

Since 2013, a total of 167 human infections with swine-origin (variant) influenza A viruses of A(H1N1)v, A(H1N2)v, and A(H3N2)v subtypes have been reported in the United States. Analysis of 147 genome sequences revealed that nearly all had S31N substitution, an M2 channel blocker-resistance marker, whereas neuraminidase inhibitor-resistance markers were not found. Two viruses had a polymerase acidic substitution (I38M or E199G) associated with decreased susceptibility to baloxavir, an inhibitor of viral cap-dependent endonuclease (CEN). Using phenotypic assays, we established subtype-specific susceptibility baselines for neuraminidase and CEN inhibitors. When compared with either baseline or CEN-sequence-matched controls, only the I38M substitution decreased baloxavir susceptibility, by 27-fold. Human monoclonal antibodies FI6v3 and CR9114 targeting the hemagglutinin's stem showed variable (0.03 to >10 µg/mL) neutralizing activity toward variant viruses, even within the same clade. Methodology and interpretation of laboratory data described in this study provide information for risk assessment and decision-making on therapeutic control measures.

摘要

自 2013 年以来,美国共报告了 167 例人类感染猪源(变异)流感 A 病毒 A(H1N1)v、A(H1N2)v 和 A(H3N2)v 亚型。对 147 个基因组序列的分析表明,几乎所有病毒都具有 S31N 取代,这是一种 M2 通道阻滞剂耐药标志物,而未发现神经氨酸酶抑制剂耐药标志物。两种病毒具有与降低对巴洛沙韦(一种病毒依赖性内切酶抑制剂)敏感性相关的聚合酶酸性取代(I38M 或 E199G)。使用表型测定法,我们建立了神经氨酸酶和 CEN 抑制剂的亚型特异性敏感性基线。与基线或 CEN 序列匹配的对照相比,仅 I38M 取代使巴洛沙韦的敏感性降低了 27 倍。针对血凝素茎的人源单克隆抗体 FI6v3 和 CR9114 对变异病毒显示出可变的(0.03 至>10 µg/mL)中和活性,即使在同一分支内也是如此。本研究中描述的实验室数据的方法和解释为风险评估和治疗控制措施的决策提供了信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3f8f/11521183/961196585d35/24-0892-F.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3f8f/11521183/961196585d35/24-0892-F.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3f8f/11521183/961196585d35/24-0892-F.jpg

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