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与抗CR2单克隆抗体偶联的低剂量抗原可在小鼠和食蟹猴中诱导快速且持久的IgG免疫反应。

Low doses of antigen coupled to anti-CR2 mAbs induce rapid and enduring IgG immune responses in mice and in cynomolgus monkeys.

作者信息

Whipple Emily C, Ditto Andrew H, Shanahan Ryan S, Gatesman Jeremy J, Little Stephen F, Taylor Ronald P, Lindorfer Margaret A

机构信息

Department of Biochemistry and Molecular Genetics, University of Virginia Health Sciences Center, Charlottesville, VA 22908, United States.

出版信息

Mol Immunol. 2007 Jan;44(4):377-88. doi: 10.1016/j.molimm.2006.02.032. Epub 2006 May 2.

Abstract

The complement system and B cell complement receptor 2 (CR2), specific for C component C3dg, play important roles in both the innate and adaptive immune response. We used hapten and protein conjugates of anti-CR2 mAbs as models for C3dg-opsonized antigens and immune complexes to examine the handling of and immune response to these reagents in mice and in non-human primates (NHP). Mice immunized and boosted i.v. with only 100 ng of Alexa 488 rat anti-mouse CR1/2 mAb 7G6 had strong IgG immune responses to the Alexa 488 hapten and to rat IgG, compared to very weak immune responses in mice treated with a comparable isotype control; larger doses of Alexa 488 mAb 7G6 did not increase the immune response. A vaccine constructed by cross-linking anthrax protective antigen to mAb 7G6 proved to be effective at low doses in generating sufficiently high titer serum IgG antibodies to neutralize anthrax lethal toxin in vitro and to protect mice from i.v. challenge with anthrax lethal toxin. When biotinylated HB135, a mouse mAb specific for human CR2, was injected i.v. into NHP, the probe manifested the same initial marginal zone B cell binding and subsequent localization to follicular dendritic cells as we have previously reported for comparable experiments in mice. Moreover, i.v. immunization of NHP with 1 microg/kg of Alexa 488 mAb HB135 promoted an IgG immune response to the Alexa 488 hapten and to mouse IgG. Taken together, these results demonstrate the efficacy of using anti-CR2 mAbs as antigen carriers for i.v. immunization with small amounts of antigens without adjuvant.

摘要

补体系统以及对补体成分C3dg具有特异性的B细胞补体受体2(CR2),在先天性和适应性免疫反应中均发挥重要作用。我们使用抗CR2单克隆抗体的半抗原和蛋白质缀合物作为C3dg调理素化抗原和免疫复合物的模型,来研究小鼠和非人类灵长类动物(NHP)对这些试剂的处理及免疫反应。静脉注射仅100 ng的Alexa 488大鼠抗小鼠CR1/2单克隆抗体7G6免疫并加强免疫的小鼠,与用类似同型对照处理的小鼠中非常微弱的免疫反应相比,对Alexa 488半抗原和大鼠IgG具有强烈的IgG免疫反应;更大剂量的Alexa 488单克隆抗体7G6并未增强免疫反应。通过将炭疽保护性抗原与单克隆抗体7G6交联构建的疫苗,在低剂量时被证明可有效产生足够高滴度的血清IgG抗体,以在体外中和炭疽致死毒素,并保护小鼠免受静脉注射炭疽致死毒素的攻击。当将生物素化的HB135(一种对人CR2具有特异性的小鼠单克隆抗体)静脉注射到NHP中时,该探针表现出与我们先前在小鼠中进行的类似实验所报道的相同的初始边缘区B细胞结合以及随后向滤泡树突状细胞的定位。此外,用1 μg/kg的Alexa 488单克隆抗体HB135对NHP进行静脉免疫,促进了对Alexa 488半抗原和小鼠IgG的IgG免疫反应。综上所述,这些结果证明了使用抗CR2单克隆抗体作为抗原载体进行无佐剂的小剂量静脉免疫的有效性。

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