戊型肝炎病毒细胞吸附模型的建立及病毒吸附区域初步研究

E.coli中表达的HEV衣壳蛋白片段P239(aa368~606)形成的类病毒颗粒与戊肝患者恢复期血清及中和单抗具有良好的反应性,较好地模拟了天然HEV病毒颗粒的表面空间结构。利用P239吸附HepG2细胞的模型来模拟HEV对宿主细胞的吸附,多株中和单抗对吸附的阻断验证了吸附的特异性。P239与多株传代细胞系的吸附结果则表明了这种特异性吸附的细胞选择性。对阻断P239吸附的线性单抗进行定位,初步确定了P239与细胞相互作用的区域:ORF2上的aa423~443很可能和病毒上的细胞膜受体结合部位非常靠近,或可能直接参与构成了病毒与细胞特异性识别的表位。此本研究为进一步研究HEV与宿主细胞的相互作用提供一定的线索。

The Establishment of Cellular Attachment Model for Hepatitis E Virus (HEV) and Its Application in the Identification of HEV Cellular Attachment Region

We have previously expressed a recombinant hepatitis E virus capsid protein p239(ORF2,aa368-606) which showed good immunogenicity and reactivity,and has been confirmed to have a simulated structure compared with native viruses. In the present study,p239 was used to simulate native HEV to investigate the attachment of HEV on host cells.Our data showed that p239 specifically attached on HepG2 cells as several HEV neutralizing monoclonal antibodies(MAbs) could block p239 attachment on cell surface.Further,by using MAbs(against) linear epitopes of p239,we identified a possible cellular binding site(aa423-443) for the capsid protein of HEV.Our data provide an important clue for the further analyzing of HEV-host cell interaction.