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一种新型抗H9N2禽流感病毒肽的鉴定与表征

Identification and characterisation of a novel anti-viral peptide against avian influenza virus H9N2.

作者信息

Rajik Mohamed, Jahanshiri Fatemeh, Omar Abdul Rahman, Ideris Aini, Hassan Sharifah Syed, Yusoff Khatijah

机构信息

Department of Microbiology, Faculty of Biotechnology and Biomolecular Sciences, University Putra Malaysia, UPM Serdang, Selangor, 43400, Malaysia.

出版信息

Virol J. 2009 Jun 5;6:74. doi: 10.1186/1743-422X-6-74.

Abstract

BACKGROUND

Avian influenza viruses (AIV) cause high morbidity and mortality among the poultry worldwide. Their highly mutative nature often results in the emergence of drug resistant strains, which have the potential of causing a pandemic. The virus has two immunologically important glycoproteins, hemagglutinin (HA), neuraminidase (NA), and one ion channel protein M2 which are the most important targets for drug discovery, on its surface. In order to identify a peptide-based virus inhibitor against any of these surface proteins, a disulfide constrained heptapeptide phage display library was biopanned against purified AIV sub-type H9N2 virus particles.

RESULTS

After four rounds of panning, four different fusion phages were identified. Among the four, the phage displaying the peptide NDFRSKT possessed good anti-viral properties in vitro and in ovo. Further, this peptide inhibited the hemagglutination activity of the viruses but showed very little and no effect on neuraminidase and hemolytic activities respectively. The phage-antibody competition assay proved that the peptide competed with anti-influenza H9N2 antibodies for the binding sites. Based on yeast two-hybrid assay, we observed that the peptide inhibited the viral replication by interacting with the HA protein and this observation was further confirmed by co-immunoprecipitation.

CONCLUSION

Our findings show that we have successfully identified a novel antiviral peptide against avian influenza virus H9N2 which act by binding with the hemagglutination protein of the virus. The broad spectrum activity of the peptide molecule against various subtypes of the avian and human influenza viruses and its comparative efficiency against currently available anti-influenza drugs are yet to be explored.

摘要

背景

禽流感病毒(AIV)在全球家禽中引起高发病率和死亡率。其高度变异的特性常常导致耐药菌株的出现,这些菌株有可能引发大流行。该病毒表面有两种具有重要免疫功能的糖蛋白,即血凝素(HA)、神经氨酸酶(NA),以及一种离子通道蛋白M2,它们是药物研发的最重要靶点。为了鉴定针对这些表面蛋白中任何一种的基于肽的病毒抑制剂,利用纯化的AIV H9N2亚型病毒颗粒对一个二硫键约束的七肽噬菌体展示文库进行了生物淘选。

结果

经过四轮淘选,鉴定出四种不同的融合噬菌体。其中,展示肽NDFRSKT的噬菌体在体外和鸡胚内具有良好的抗病毒特性。此外,该肽抑制了病毒的血凝活性,但分别对神经氨酸酶和溶血活性显示出极小的影响且无作用。噬菌体 - 抗体竞争试验证明该肽与抗H9N2流感抗体竞争结合位点。基于酵母双杂交试验,我们观察到该肽通过与HA蛋白相互作用抑制病毒复制,并且通过免疫共沉淀进一步证实了这一观察结果。

结论

我们的研究结果表明,我们已成功鉴定出一种针对禽流感病毒H9N2的新型抗病毒肽,其通过与病毒的血凝蛋白结合发挥作用。该肽分子对禽和人流感病毒各种亚型的广谱活性及其与现有抗流感药物相比的效率还有待探索。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/905a/2700090/6957958f598f/1743-422X-6-74-1.jpg

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