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HIV-1 Env-Specific Memory and Germinal Center B Cells in C57BL/6 Mice

机译:C57BL / 6小鼠的HIV-1 Env特异性记忆和生殖中心B细胞

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摘要

Continued efforts to define the immunogenic properties of the HIV-1 envelope glycoproteins (Env) are needed to elicit effective antibody (Ab) responses by vaccination. HIV-1 is a highly neutralization-resistant virus due to conformational and glycan shielding of conserved Ab determinants on the virus spike. Elicitation of broadly neutralizing Abs that bind poorly accessible epitope regions on Env is therefore extremely challenging and will likely require selective targeting of specific sub-determinants. To evaluate such approaches there is a pressing need for in vivo studies in both large and small animals, including mice. Currently, most mouse immunization studies are performed in the BALB/c strain; however, the C57BL/6 strain offers improved possibilities for mechanistic studies due to the availability of numerous knock-out strains on this genetic background. Here, we compared Env immunogenicity in BALB/c and C57BL/6 mice and found that the magnitude of the antigen-specific response was somewhat lower in C57BL/6 than in BALB/c mice by ELISA but not significantly different by B cell ELISpot measurements. We then established protocols for the isolation of single Env-specific memory B cells and germinal center (GC) B cells from immunized C57BL/6 mice to facilitate future studies of the elicited response at the monoclonal Ab level. We propose that these protocols can be used to gain an improved understanding of the early recruitment of Env-specific B cells to the GC as well as the archiving of such responses in the memory B cell pool following immunization.
机译:需要持续的努力来定义HIV-1包膜糖蛋白(Env)的免疫原性,以通过疫苗接种引发有效的抗体(Ab)反应。 HIV-1是一种高度抗中和性的病毒,这是由于病毒尖峰上保守的Ab决定簇的构象和糖基被屏蔽。因此,结合结合在Env上难以接近的表位区域的广泛中和的Abs的提纯极具挑战性,可能需要选择性靶向特定的亚决定簇。为了评估这种方法,迫切需要在大型和小型动物(包括小鼠)中进行体内研究。目前,大多数小鼠免疫研究都是在BALB / c株中进行的;但是,由于在这种遗传背景下可获得大量敲除菌株,因此C57BL / 6菌株为机理研究提供了改进的可能性。在这里,我们比较了BALB / c和C57BL / 6小鼠的Env免疫原性,发现通过ELISA,C57BL / 6的抗原特异性应答幅度比BALB / c小鼠低,但是通过B细胞ELISpot测量没有显着差异。然后,我们建立了从免疫的C57BL / 6小鼠中分离单个Env特异性记忆B细胞和生发中心(GC)B细胞的协议,以促进在单克隆抗体水平上引起的应答的进一步研究。我们建议可以使用这些协议来更好地了解Env特异性B细胞向GC的早期募集以及免疫后在记忆B细胞池中保存此类应答。

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