Wei-Yun Wholey, Alexander R Meyer, Sekou-Tidiane Yoda, James L Mueller, Raisa Mathenge, Bryce Chackerian, Julie Zikherman, Wei Cheng
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引用次数: 0
摘要
许多病毒感染后都会迅速诱导产生类调控中和抗体(nAb)。然而,由于病毒中存在多种成分,病毒感染引发 nAb 反应的精确生化和生物物理信号仍未得到充分定义。在本研究中,我们利用一个合成病毒样结构的还原系统,证明病毒大小脂质体上的外来蛋白可作为独立的危险信号,在没有 T 细胞帮助或 TLR 的情况下启动类别开关 nAb 反应,但需要 CD19。引入内部核酸(iNAs)后,就不再需要 CD19,降低了诱发抗体反应所需的表位密度(ED),并将这些结构转化为强效免疫原,其诱发强抗体特异性 IgG 的能力可与传统病毒样颗粒相媲美。早在免疫后第 5 天,在剂量低至 100 毫微克的情况下,含有 iNAs 并装饰有少量表面 Ag 分子的结构就能诱导小鼠体内所有 IgG 亚类的抗体,并再现了在活病毒感染中长期观察到的 IgG2a/2c 限制。这些发现揭示了小鼠 nAb 反应的共同机制。高ED能够但并非驱动抗体分泌的必要条件。相反,即使是几个表面Ag分子,当与这些结构中的核酸结合时,也能引发强烈的IgG分泌。因此,诱导单个 B 细胞产生 IgG 的信号阈值是由来自表面 ED 和病毒颗粒免疫原中 iNA 的双重信号设定的。
An Integrated Signaling Threshold Initiates IgG Response toward Virus-like Immunogens.
Class-switched neutralizing Ab (nAb) production is rapidly induced upon many viral infections. However, due to the presence of multiple components in virions, the precise biochemical and biophysical signals from viral infections that initiate nAb responses remain inadequately defined. Using a reductionist system of synthetic virus-like structures, in this study, we show that a foreign protein on a virion-sized liposome can serve as a stand-alone danger signal to initiate class-switched nAb responses without T cell help or TLR but requires CD19. Introduction of internal nucleic acids (iNAs) obviates the need for CD19, lowers the epitope density (ED) required to elicit the Ab response, and transforms these structures into highly potent immunogens that rival conventional virus-like particles in their ability to elicit strong Ag-specific IgG. As early as day 5 after immunization, structures harboring iNAs and decorated with just a few molecules of surface Ag at doses as low as 100 ng induced all IgG subclasses of Ab in mice and reproduced the IgG2a/2c restriction that is long observed in live viral infections. These findings reveal a shared mechanism for the nAb response in mice. High ED is capable but not necessary for driving Ab secretion. Instead, even a few molecules of surface Ag, when combined with nucleic acids within these structures, can trigger strong IgG production. As a result, the signaling threshold for induction of IgG in individual B cells is set by dual signals originating from both ED on the surface and the presence of iNAs within viral particulate immunogens.
期刊介绍:
The JI publishes novel, peer-reviewed findings in all areas of experimental immunology, including innate and adaptive immunity, inflammation, host defense, clinical immunology, autoimmunity and more. Special sections include Cutting Edge articles, Brief Reviews and Pillars of Immunology. The JI is published by The American Association of Immunologists (AAI)