腺病毒血清型依赖性Gas6结合对I型干扰素反应的抑制作用。
Inhibition of type I interferon responses by adenovirus serotype-dependent Gas6 binding.
作者信息
Nidetz Natalie F, Gallagher Tom M, Wiethoff Christopher M
机构信息
Loyola University Chicago, 2016 S. First Avenue, Maywood, IL 60153, USA.
出版信息
Virology. 2018 Feb;515:150-157. doi: 10.1016/j.virol.2017.12.016. Epub 2017 Dec 27.
Abstract
The clinical use of many adenovirus vaccine vectors (AdVs) is limited by the presence of pre-existing antibodies in human populations, which prevent common AdVs from transducing cells and expressing immunogenic gene products. Rare serotype AdVs, such as HAdV-28D can bypass pre-existing immunity. However, rare AdVs stimulate high-levels of type I interferon (IFN), which suppresses antigenic gene expression and therefore limits immunogenicity. Recent studies identified Gas6 as a factor that connects enveloped viruses to host-cell receptor tyrosine kinases, in turn generating signaling cascades that antagonize type I IFN responses. We discovered that Gas6 bound to the fiber proteins of common AdV serotypes, such as HAdV-5C, with a higher affinity than rare HAd-28D fibers. AdV-associated Gas6 suppressed IFN production by common AdVs and enhanced long-term expression of AdV encoded genes. We hypothesize that rare AdV serotypes might be engineered to include Gas6 binding motifs, thereby generating novel vectors that are more effective.
摘要
许多腺病毒疫苗载体(AdV)的临床应用受到人群中预先存在抗体的限制,这些抗体可阻止常见AdV转导细胞并表达免疫原性基因产物。罕见血清型AdV,如HAdV-28D,可绕过预先存在的免疫。然而,罕见AdV会刺激高水平的I型干扰素(IFN),从而抑制抗原基因表达,进而限制免疫原性。最近的研究确定Gas6是一种将包膜病毒与宿主细胞受体酪氨酸激酶连接起来的因子,进而产生拮抗I型IFN反应的信号级联。我们发现,Gas6与常见AdV血清型(如HAdV-5C)的纤维蛋白结合,其亲和力高于罕见的HAd-28D纤维。与AdV相关的Gas6可抑制常见AdV产生IFN,并增强AdV编码基因的长期表达。我们推测,罕见AdV血清型可经过改造以包含Gas6结合基序,从而产生更有效的新型载体。
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