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描述羊口疮病毒(副痘病毒属)的免疫刺激成分。

Characterization of immunostimulatory components of orf virus (parapoxvirus ovis).

机构信息

Institute of Medical Immunology and Berlin-Brandenburg Center for Regenerative Therapies (BCRT), Charité - Universitätsmedizin Berlin, Berlin, Germany.

Bayer HealthCare AG, Leverkusen, Germany.

出版信息

J Gen Virol. 2011 Jul;92(Pt 7):1571-1584. doi: 10.1099/vir.0.028894-0. Epub 2011 Feb 23.

Abstract

Inactivated orf virus (ORFV, parapoxvirus ovis) induces antiviral activity in animal models of acute and chronic viral infections and exerts strong effects on human immune cells. ORFV activates antigen presenting cells (APC) via CD14 and, probably, Toll-like receptor signalling, and triggers the release of IFN-γ that has been identified as the key mediator of the antiviral activity. After delineating virus proteins as being the most likely active constituent, we aimed to characterize the ORFV proteins responsible for the therapeutic effect. By using a vaccinia virus/ORFV expression library we identified several multi-gene DNA fragments with strong immunomodulatory activity. Together these fragments contain 27 ORFs. The encoded proteins are related to virion structure and transcription but are otherwise unrelated. Two proteins were separately expressed and purified, and demonstrated immunostimulatory activity. Gene expression profiles induced by ORFV and the identified fragments were investigated by microarray analysis. Interestingly, all active fragments induced a similar gene-expression pattern, differing only in quantitative aspects. Obviously, several proteins of ORFV activate similar cellular pathways, modulating APC to generate a strong T-helper 1-dominated immune response. This was balanced by additional induction of immune dampening mechanisms, suggesting regulatory differences compared to single cytokine therapies. We conclude that ORFV may have the potential to enrich the armamentarium of antiviral therapies.

摘要

灭活口疮病毒(ORFV,羊痘病毒)在急性和慢性病毒感染的动物模型中诱导抗病毒活性,并对人类免疫细胞产生强烈影响。ORFV 通过 CD14 并可能通过 Toll 样受体信号激活抗原提呈细胞 (APC),并触发 IFN-γ 的释放,IFN-γ 已被确定为抗病毒活性的关键介质。在将病毒蛋白描绘为最有可能的有效成分后,我们旨在表征负责治疗效果的 ORFV 蛋白。通过使用痘苗病毒/ORFV 表达文库,我们鉴定了几个具有强烈免疫调节活性的多基因 DNA 片段。这些片段共同包含 27 个 ORF。编码的蛋白质与病毒粒子结构和转录有关,但彼此无关。两种蛋白质分别表达和纯化,并表现出免疫刺激活性。通过微阵列分析研究了 ORFV 和鉴定的片段诱导的基因表达谱。有趣的是,所有活性片段诱导出相似的基因表达模式,仅在定量方面有所不同。显然,ORFV 的几种蛋白激活相似的细胞途径,调节 APC 以产生强烈的 Th1 优势免疫反应。这通过额外诱导免疫抑制机制得到平衡,表明与单一细胞因子治疗相比存在调节差异。我们得出结论,ORFV 可能具有丰富抗病毒治疗方法的潜力。

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