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免疫功能低下的韩国患者感染 hMPV,亚谱系 B.1.3,在特考韦瑞治疗期间出现获得性耐药突变,导致病毒持续排出。

Prolonged viral shedding in an immunocompromised Korean patient infected with hMPXV, sub-lineage B.1.3, with acquired drug resistant mutations during tecovirimat treatment.

机构信息

Division of High-risk Pathogens, Bureau of Infectious Disease Diagnosis Control, Korea Disease Control and Prevention Agency, Cheongju, South Korea.

出版信息

J Med Virol. 2024 Mar;96(3):e29536. doi: 10.1002/jmv.29536.

DOI:10.1002/jmv.29536
PMID:38488495
Abstract

Following the worldwide surge in mpox (monkeypox) in 2022, cases have persisted in Asia, including South Korea, and sexual contact is presumed as the predominant mode of transmission, with a discernible surge in prevalence among immunocompromised patients. Drugs such as tecovirimat can result in drug-resistant mutations, presenting obstacles to treatment. This study aimed to ascertain the presence of tecovirimat-related resistant mutations through genomic analysis of the monkeypox virus isolated from a reported case involving prolonged viral shedding in South Korea. Here, tecovirimat-resistant mutations, previously identified in the B.1 clade, were observed in the B.1.3 clade, predominant in South Korea. These mutations exhibited diverse patterns across different samples from the same patient and reflected the varied distribution of viral subpopulations in different anatomical regions. The A290V and A288P mutant strains we isolated hold promise for elucidating these mechanisms, enabling a comprehensive analysis of viral pathogenesis, replication strategies, and host interactions. Our findings imply that acquired drug-resistant mutations, may present a challenge to individual patient treatment. Moreover, they have the potential to give rise to transmitted drug-resistant mutations, thereby imposing a burden on the public health system. Consequently, the meticulous genomic surveillance among immunocompromised patients, conducted in this research, assumes paramount importance.

摘要

在 2022 年全球猴痘(猴痘)疫情爆发后,亚洲(包括韩国)仍有病例持续出现,性接触被认为是主要传播途径,免疫功能低下患者的发病率明显上升。特考韦瑞玛等药物可能会导致耐药突变,给治疗带来障碍。本研究旨在通过对韩国报告的一例病毒持续排出时间较长的病例中分离的猴痘病毒进行基因组分析,确定是否存在与特考韦瑞玛相关的耐药突变。在韩国流行的 B.1.3 分支中观察到了先前在 B.1 分支中发现的特考韦瑞玛耐药突变。这些突变在同一患者的不同样本中表现出不同的模式,反映了不同解剖部位病毒亚群的不同分布。我们分离的 A290V 和 A288P 突变株有助于阐明这些机制,可全面分析病毒发病机制、复制策略和宿主相互作用。我们的研究结果表明,获得性耐药突变可能会给个体患者的治疗带来挑战。此外,它们还有可能产生传播性耐药突变,从而给公共卫生系统带来负担。因此,本研究中对免疫功能低下患者进行的细致的基因组监测显得尤为重要。

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引用本文的文献

1
Tecovirimat is active against various MPXV strains, while cidofovir, brincidofovir, trifluridine, and gemcitabine have no detectable MPXV-specific antiviral activity.替考韦瑞玛对多种猴痘病毒(MPXV)毒株具有活性,而西多福韦、布林西多福韦、曲氟尿苷和吉西他滨则未检测到猴痘病毒特异性抗病毒活性。
Virus Res. 2025 Aug 12;360:199615. doi: 10.1016/j.virusres.2025.199615.
2
Structural insights into tecovirimat antiviral activity and poxvirus resistance.对替考韦瑞玛抗病毒活性和痘病毒耐药性的结构见解。
Nat Microbiol. 2025 Mar;10(3):734-748. doi: 10.1038/s41564-025-01936-6. Epub 2025 Feb 12.