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霍乱毒素 A1-DD 佐剂的独特作用:促进长期血浆细胞和记忆 B 细胞的发育。

A unique role of the cholera toxin A1-DD adjuvant for long-term plasma and memory B cell development.

机构信息

Department of Microbiology and Immunology, Mucosal Immunobiology and Vaccine Center, Institute of Biomedicine, University of Gothenburg, Gothenburg, Sweden.

出版信息

J Immunol. 2011 Feb 1;186(3):1399-410. doi: 10.4049/jimmunol.1002881. Epub 2011 Jan 3.

Abstract

Adjuvants have traditionally been appreciated for their immunoenhancing effects, whereas their impact on immunological memory has largely been neglected. In this paper, we have compared three mechanistically distinct adjuvants: aluminum salts (Alum), Ribi (monophosphoryl lipid A), and the cholera toxin A1 fusion protein CTA1-DD. Their influence on long-term memory development was dramatically different. Whereas a single immunization i.p. with 4-hydroxy-3-nitrophenyl acetyl (NP)-chicken γ-globulin and adjuvant stimulated serum anti-NP IgG titers that were comparable at 5 wk, CTA1-DD-adjuvanted responses were maintained for >16 mo with a half-life of anti-NP IgG ∼36 wk, but <15 wk after Ribi or Alum. A CTA1-DD dose-dependent increase in germinal center (GC) size and numbers was found, with >60% of splenic B cell follicles hosting GC at an optimal CTA1-DD dose. Roughly 7% of these GC were NP specific. This GC-promoting effect correlated well with the persistence of long-term plasma cells in the bone marrow and memory B cells in the spleen. CTA1-DD also facilitated increased somatic hypermutation and affinity maturation of NP-specific IgG Abs in a dose-dependent fashion, hence arguing that large GC not only promotes higher Ab titers but also high-quality Ab production. Adoptive transfer of splenic CD80(+), but not CD80(-), B cells, at 1 y after immunization demonstrated functional long-term anti-NP IgG and IgM memory cells. To our knowledge, this is the first report to specifically compare and document that adjuvants can differ considerably in their support of long-term immune responses. Differential effects on the GC reaction appear to be the basis for these differences.

摘要

佐剂传统上因其免疫增强作用而受到重视,而其对免疫记忆的影响在很大程度上被忽视了。在本文中,我们比较了三种机制上不同的佐剂:铝盐(Alum)、Ribi(单磷酰脂质 A)和霍乱毒素 A1 融合蛋白 CTA1-DD。它们对长期记忆发展的影响有很大的不同。单次腹腔注射 4-羟基-3-硝基苯乙酰(NP)-鸡 γ-球蛋白和佐剂可刺激血清抗 NP IgG 滴度在 5 周时相当,但 CTA1-DD 佐剂的反应可维持>16 个月,抗 NP IgG 的半衰期为 36 周,但在 Ribi 或 Alum 后<15 周。发现 CTA1-DD 剂量依赖性增加生发中心(GC)的大小和数量,在最佳 CTA1-DD 剂量下,超过 60%的脾 B 细胞滤泡含有 GC。大约 7%的 GC 是 NP 特异性的。这种 GC 促进作用与长期浆细胞在骨髓中的存在和记忆 B 细胞在脾脏中的存在密切相关。CTA1-DD 还以剂量依赖的方式促进 NP 特异性 IgG Abs 的体细胞超突变和亲和力成熟,因此认为大 GC 不仅促进更高的 Ab 滴度,而且还促进高质量的 Ab 产生。免疫后 1 年,脾 CD80(+)而非 CD80(-)B 细胞的过继转移显示了功能性的长期抗 NP IgG 和 IgM 记忆细胞。据我们所知,这是第一个专门比较和证明佐剂在支持长期免疫反应方面可以有很大差异的报告。对 GC 反应的不同影响似乎是这些差异的基础。

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