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从乌干达家禽中分离的禽流感 A(H9N2)病毒的遗传进化揭示了哺乳动物宿主适应、毒力增加和对巴洛沙韦敏感性降低的证据。

Genetic Evolution of Avian Influenza A (H9N2) Viruses Isolated from Domestic Poultry in Uganda Reveals Evidence of Mammalian Host Adaptation, Increased Virulence and Reduced Sensitivity to Baloxavir.

机构信息

Makerere University Walter Reed Project, Kampala P.O. Box 16524, Uganda.

St Jude Children's Research Hospital, MS330, Memphis, TN 38105, USA.

出版信息

Viruses. 2022 Sep 18;14(9):2074. doi: 10.3390/v14092074.

Abstract

A (H9N2) avian influenza A viruses were first detected in Uganda in 2017 and have since established themselves in live bird markets. The aim of this study was to establish the subsequent genetic evolution of H9N2 viruses in Uganda. Cloacal samples collected from live bird market stalls in Kampala from 2017 to 2019 were screened by RT-PCR for influenza A virus and H9N2 viruses were isolated in embryonated eggs. One hundred and fifty H9N2 isolates were subjected to whole genome sequencing on the Illumina MiSeq platform. The sequence data analysis and comparison with contemporary isolates revealed that the virus was first introduced into Uganda in 2014 from ancestors in the Middle East. There has since been an increase in nucleotide substitutions and reassortments among the viruses within and between live bird markets, leading to variations in phylogeny of the different segments, although overall diversity remained low. The isolates had several mutations such as HA-Q226L and NS-I106M that enable mammalian host adaptation, NP-M105V, PB1-D3V, and M1-T215A known for increased virulence/pathogenicity and replication, and PA-E199D, NS-P42S, and M2-S31N that promote drug resistance. The PA-E199D substitution in particular confers resistance to the endonuclease inhibitor Baloxavir acid, which is one of the new anti-influenza drugs. Higher EC50 was observed in isolates with a double F105L+E199D substitution that may suggest a possible synergistic effect. These H9N2 viruses have established an endemic situation in live bird markets in Uganda because of poor biosecurity practices and therefore pose a zoonotic threat. Regular surveillance is necessary to further generate the needed evidence for effective control strategies and to minimize the threats.

摘要

(H9N2)禽流感病毒于 2017 年在乌干达首次被检测到,此后已在活禽市场立足。本研究旨在确定乌干达 H9N2 病毒的后续遗传进化。2017 年至 2019 年,从坎帕拉活禽市场摊位采集的泄殖腔样本通过 RT-PCR 筛查流感病毒,并用鸡胚分离 H9N2 病毒。对 150 株 H9N2 分离株进行 Illumina MiSeq 平台全基因组测序。序列数据分析并与同期分离株比较显示,该病毒于 2014 年首次从中东的祖先传入乌干达。此后,活禽市场内和活禽市场之间的病毒发生了核苷酸替换和重配,导致不同片段的系统发生发生了变化,尽管整体多样性仍然较低。分离株有几个突变,如 HA-Q226L 和 NS-I106M,这些突变使病毒能够适应哺乳动物宿主,NP-M105V、PB1-D3V 和 M1-T215A 已知会增加病毒的毒力/致病性和复制能力,而 PA-E199D、NS-P42S 和 M2-S31N 则会促进耐药性。特别是 PA-E199D 的突变赋予了对内切酶抑制剂巴洛沙韦酸的耐药性,巴洛沙韦酸是一种新型抗流感药物。在具有双 F105L+E199D 突变的分离株中观察到更高的 EC50,这可能表明存在协同作用。由于生物安全措施不佳,这些 H9N2 病毒在乌干达的活禽市场已建立了地方性流行情况,因此构成了人畜共患病威胁。需要定期进行监测,以进一步提供有效控制策略所需的证据,并最大程度地减少威胁。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/579b/9505320/2a5d77d4bfdb/viruses-14-02074-g0A1.jpg

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