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免疫功能低下动物中药物敏感性及耐药性严重急性呼吸综合征冠状病毒2出现的可能性。

Drug susceptibility and the potential for drug-resistant SARS-CoV-2 emergence in immunocompromised animals.

作者信息

Kiso Maki, Uraki Ryuta, Yamayoshi Seiya, Imai Masaki, Kawaoka Yoshihiro

机构信息

Pandemic Preparedness, Infection and Advanced Research Center (UTOPIA), The University of Tokyo, Tokyo 108-8639, Japan.

Division of Virology, Institute of Medical Science, University of Tokyo, Tokyo 108-8639, Japan.

出版信息

iScience. 2024 Aug 17;27(9):110729. doi: 10.1016/j.isci.2024.110729. eCollection 2024 Sep 20.

Abstract

The reduced susceptibility of mRNA vaccines and diminished neutralizing activity of therapeutic monoclonal antibodies against Omicron variants, including BQ.1.1, XBB, and their descendants, highlight the importance of antiviral therapies. Here, we assessed the efficacy of two antivirals, molnupiravir, targeting a viral RNA-dependent RNA polymerase, and nirmatrelvir, targeting a main protease, against BQ.1.1 in hamsters. We found that prophylactic or therapeutic treatment with either drug significantly reduced the viral load in the lungs of infected hamsters. We also evaluated the risk of emergence of drug-resistant viruses in immunocompromised hamsters. Although 13 days of drug treatment reduced viral titers, the immunocompromised hosts could not completely clear the virus. Viruses isolated from drug-treated immunocompromised hamsters did not show reduced susceptibility to the drugs. Molnupiravir and nirmatrelvir remain effective against variants with reduced susceptibility to monoclonal antibodies and mRNA vaccine-induced antibodies, with limited emergence of drug-resistant variants under the conditions tested.

摘要

mRNA疫苗的敏感性降低,以及治疗性单克隆抗体对包括BQ.1.1、XBB及其后代在内的奥密克戎变体的中和活性减弱,凸显了抗病毒疗法的重要性。在此,我们评估了两种抗病毒药物(靶向病毒RNA依赖性RNA聚合酶的莫努匹拉韦和靶向主要蛋白酶的奈玛特韦)对仓鼠体内BQ.1.1的疗效。我们发现,用这两种药物进行预防性或治疗性治疗,均可显著降低受感染仓鼠肺部的病毒载量。我们还评估了免疫功能低下的仓鼠中出现耐药病毒的风险。尽管13天的药物治疗降低了病毒滴度,但免疫功能低下的宿主无法完全清除病毒。从接受药物治疗的免疫功能低下的仓鼠中分离出的病毒对这些药物的敏感性并未降低。在测试条件下,莫努匹拉韦和奈玛特韦对单克隆抗体和mRNA疫苗诱导抗体敏感性降低的变体仍然有效,耐药变体的出现有限。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6809/11402253/28ab72d24c39/fx1.jpg

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