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抗体针对蓖麻毒素结合亚基(RTB)赋予的蓖麻毒素保护性免疫。

Protective immunity to ricin toxin conferred by antibodies against the toxin's binding subunit (RTB).

机构信息

Department of Biomedical Sciences, University at Albany School of Public Health, Albany, NY 12201, USA.

出版信息

Vaccine. 2011 Oct 19;29(45):7925-35. doi: 10.1016/j.vaccine.2011.08.075. Epub 2011 Aug 26.

Abstract

The B subunit (RTB) of ricin toxin is a galactose-/N-acetyl galactosamine-specific lectin that promotes attachment and entry of ricin into host cells. RTB is also the archetype of the so-called R-type lectin family, whose members include haemagglutinins of botulinum neurotoxin (BoNT) progenitor toxins, as well as the binding subunits of cytolethal distending toxins. Although RTB is an appealing subunit vaccine candidate, as well as a potential target for immunotherapeutics, the degree to which RTB immunization elicits protective antibodies against ricin toxin remains unresolved. To address this issue, groups of mice were immunized with RTB and then challenged with 5×LD(50)s of ricin administered intraperitoneally. Despite high RTB-specific serum antibody titers, groups of RTB immunized mice were only partially immune to ricin challenge. Analysis of a collection of RTB-specific B cell hybridomas suggested that only a small fraction of antibodies against RTB have demonstrable neutralizing activity. Two RTB-specific neutralizing monoclonal IgG(1) antibodies, 24B11 and SylH3, when passively administered to mice, were sufficient to protect the animals against a 5×LD(50) dose of ricin. Both 24B11 and SylH3 blocked ricin attachment to terminal galactose residues and prevented toxin binding to the surfaces of bone marrow-derived macrophages (BMM), suggesting that they function by steric hindrance and recognize epitopes located on RTB's carbohydrate recognition sub-domains (1α or 2γ). These data raise the possibility of using specific RTB sub-domains, rather than RTB itself, as antigens to more efficiently elicit neutralizing antibodies and protective immunity against ricin.

摘要

蓖麻毒素的 B 亚基(RTB)是一种半乳糖/N-乙酰半乳糖胺特异性凝集素,可促进蓖麻毒素进入宿主细胞。RTB 也是所谓的 R 型凝集素家族的原型,其成员包括肉毒神经毒素(BoNT)前体毒素的血凝素,以及细胞毒性扩张毒素的结合亚基。尽管 RTB 是一种有吸引力的亚单位疫苗候选物,也是免疫治疗的潜在靶点,但 RTB 免疫引发针对蓖麻毒素的保护性抗体的程度仍未解决。为了解决这个问题,一组小鼠用 RTB 免疫,然后用腹腔内注射 5×LD(50)的蓖麻毒素进行挑战。尽管 RTB 特异性血清抗体滴度很高,但 RTB 免疫组的小鼠仅对蓖麻毒素的挑战具有部分免疫力。对一组 RTB 特异性 B 细胞杂交瘤的分析表明,针对 RTB 的抗体只有一小部分具有可证明的中和活性。两种 RTB 特异性中和单克隆 IgG(1)抗体 24B11 和 SylH3,被动给予小鼠时,足以保护动物免受 5×LD(50)剂量的蓖麻毒素的侵害。24B11 和 SylH3 均能阻止蓖麻毒素与末端半乳糖残基结合,并防止毒素与骨髓来源的巨噬细胞(BMM)表面结合,这表明它们通过空间位阻起作用,并识别 RTB 的碳水化合物识别亚结构域(1α或 2γ)上的表位。这些数据提出了使用特定的 RTB 亚结构域而不是 RTB 本身作为抗原更有效地引发针对蓖麻毒素的中和抗体和保护性免疫的可能性。

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