首页> 美国卫生研究院文献>Journal of Virology >Dendritic Cell Internalization of Foot-and-Mouth Disease Virus: Influence of Heparan Sulfate Binding on Virus Uptake and Induction of the Immune Response
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Dendritic Cell Internalization of Foot-and-Mouth Disease Virus: Influence of Heparan Sulfate Binding on Virus Uptake and Induction of the Immune Response

机译:口蹄疫病毒的树突状细胞内在化:硫酸乙酰肝素结合对病毒摄取和免疫应答诱导的影响

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摘要

Dendritic cells (DC), which are essential for inducing and regulating immune defenses and responses, represent the critical target for vaccines against pathogens such as foot-and-mouth disease virus (FMDV). Although it is clear that FMDV enters epithelial cells via integrins, little is known about FMDV interaction with DC. Accordingly, DC internalization of FMDV antigen was analyzed by comparing vaccine virus dominated by heparan sulfate (HS)-binding variants with FMDV lacking HS-binding capacity. The internalization was most efficient with the HS-binding virus, employing diverse endocytic pathways. Moreover, internalization relied primarily on HS binding. Uptake of non-HS-binding virus by DC was considerably less efficient, so much so that it was often difficult to detect virus interacting with the DC. The HS-binding FMDV replicated in DC, albeit transiently, which was demonstrable by its sensitivity to cycloheximide treatment and the short duration of infectious virus production. There was no evidence that the non-HS-binding virus replicated in the DC. These observations on virus replication may be explained by the activities of viral RNA in the DC. When DC were transfected with infectious RNA, only 1% of the translated viral proteins were detected. Nevertheless, the transfected cells, and DC which had internalized live virus, did present antigen to lymphocytes, inducing an FMDV-specific immunoglobulin G response. These results demonstrate that DC internalization of FMDV is most efficient for vaccine virus with HS-binding capacity, but HS binding is not an exclusive requirement. Both non-HS-binding virus and infectious RNA interacting with DC induce specific immune responses, albeit less efficiently than HS-binding virus.
机译:树突状细胞(DC)是诱导和调节免疫防御和反应必不可少的,它代表了针对诸如口蹄疫病毒(FMDV)等病原体的疫苗的关键目标。尽管很明显FMDV通过整联蛋白进入上皮细胞,但是关于FMDV与DC的相互作用知之甚少。因此,通过比较以硫酸乙酰肝素(HS)结合变体为主的疫苗病毒与缺乏HS结合能力的FMDV来分析FMDV抗原的DC内在化。使用多种内吞途径,HS结合病毒的内化作用最有效。此外,内部化主要依赖于HS绑定。 DC对非HS结合病毒的吸收效率相当低,以至于通常很难检测与DC相互作用的病毒。结合HS的FMDV虽在DC中短暂复制,但其对环己酰亚胺治疗的敏感性和感染性病毒的生产时间短证明了这一点。没有证据表明非HS结合病毒在DC中复制。这些关于病毒复制的观察结果可以通过DC中病毒RNA的活性来解释。当DC用感染性RNA转染时,仅检测到1%的翻译病毒蛋白。然而,转染的细胞和内在活病毒的DC确实向淋巴细胞呈递抗原,从而诱导了FMDV特异性免疫球蛋白G应答。这些结果表明,FMDV的DC内在化对于具有HS结合能力的疫苗病毒最有效,但HS结合并不是唯一的要求。尽管与HS结合病毒相比,非HS结合病毒和与DC相互作用的传染性RNA均可诱导特异性免疫反应。

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