Interferon-alpha and MxA inhibit BK polyomavirus replication by interaction with polyomavirus large T antigen

IF 4.1 3区 医学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
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引用次数: 0

Abstract

Introduction

BK Polyomavirus (BKPyV) infection is a common complication in kidney transplant recipients and can result in poor outcomes and graft failure. Currently, there is no known effective antiviral agent. This study investigated the possible antiviral effects of Interferon alpha (IFNα) and its induced protein, MxA, against BKPyV.

Methods

In vitro cell culture experiments were conducted using human primary renal proximal tubular epithelial cells (HRPTECs). We also did animal studies using Balb/c mice with unilateral kidney ischemic reperfusion injury.

Results

Our results demonstrated that IFNα effectively inhibited BKPyV in vitro and murine polyomavirus in animal models. Additionally, IFNα and MxA were found to suppress BKPyV TAg and VP1 production. Silencing MxA attenuated the antiviral efficacy of IFNα. We observed that MxA interacted with BKPyV TAg, causing it to remain in the cytosol and preventing its nuclear translocation. To determine MxA's essential domain for its antiviral activities, different mutant MxA constructs were generated. The MxA mutant K83A retained its interaction with BKPyV TAg, and its antiviral effects were intact. The MxA T103A mutant, on the other hand, abolished GTPase activity, lost its protein-protein interaction with BKPyV TAg, and lost its antiviral effect.

Conclusion

IFNα and its downstream protein, MxA, have potent antiviral properties against BKPyV. Furthermore, our findings indicate that the interaction between MxA and BKVPyV TAg plays a crucial role in determining the anti-BKPyV effects of MxA.

α干扰素和MxA通过与多瘤病毒大T抗原相互作用抑制BK多瘤病毒的复制
导言BK 多瘤病毒(BKPyV)感染是肾移植受者常见的并发症,可导致不良预后和移植失败。目前,尚无有效的抗病毒药物。本研究调查了α干扰素(IFNα)及其诱导蛋白MxA对BKPyV可能产生的抗病毒作用。方法使用人原代肾近曲小管上皮细胞(HRPTECs)进行体外细胞培养实验。结果我们的研究结果表明,IFNα 在体外能有效抑制 BKPyV,在动物模型中能有效抑制鼠多瘤病毒。此外,还发现 IFNα 和 MxA 可抑制 BKPyV TAg 和 VP1 的产生。我们观察到 MxA 与 BKPyV TAg 相互作用,使其停留在细胞质中并阻止其核转运。为了确定MxA抗病毒活性的关键结构域,我们生成了不同的突变MxA构建体。MxA 突变体 K83A 保留了与 BKPyV TAg 的相互作用,其抗病毒作用也完好无损。结论IFNα及其下游蛋白MxA对BKPyV有很强的抗病毒作用。此外,我们的研究结果表明,MxA 与 BKVPyV TAg 之间的相互作用在决定 MxA 的抗 BKPyV 作用方面起着至关重要的作用。
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来源期刊
Biomedical Journal
Biomedical Journal Medicine-General Medicine
CiteScore
11.60
自引率
1.80%
发文量
128
审稿时长
42 days
期刊介绍: Biomedical Journal publishes 6 peer-reviewed issues per year in all fields of clinical and biomedical sciences for an internationally diverse authorship. Unlike most open access journals, which are free to readers but not authors, Biomedical Journal does not charge for subscription, submission, processing or publication of manuscripts, nor for color reproduction of photographs. Clinical studies, accounts of clinical trials, biomarker studies, and characterization of human pathogens are within the scope of the journal, as well as basic studies in model species such as Escherichia coli, Caenorhabditis elegans, Drosophila melanogaster, and Mus musculus revealing the function of molecules, cells, and tissues relevant for human health. However, articles on other species can be published if they contribute to our understanding of basic mechanisms of biology. A highly-cited international editorial board assures timely publication of manuscripts. Reviews on recent progress in biomedical sciences are commissioned by the editors.
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