胸腺非依赖性抗原(NIP-ficoll)启动后的免疫记忆。4-羟基-5-碘-3-硝基苯乙酰偶联蔗糖和环氧氯丙烷聚合物。

M. Hurme
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引用次数: 5

摘要

研究了小鼠脾碎片体外抗nip(4-羟基-5-碘-3-硝基苯基乙酰基)反应的能力。这些片段来自未引物的NIP-Ficoll(蔗糖和环氧氯丙烷的聚合物)或NIP-CG(鸡球蛋白)引物小鼠。未引物的C57BL/6小鼠脾脏片段对NIP-Ficoll具有良好的抗nip反应,而CBA片段则没有。用NIP-Ficoll引发CBA片段反应,用相同抗原刺激C57BL/6片段时,CBA片段反应略有增强。这种记忆效应只有在小剂量启动后才会出现。用NIP- ficoll刺激小鼠,使其脾脏片段对NIP蛋白偶联物(NIP- cg)产生反应,但这种作用仅在高剂量启动后才出现。不同种类的免疫球蛋白在体外原发性和继发性应答中的抗体类分布和出现动力学相似。IgM、IgA和IgG的反应在第8天达到高峰,IgG在初次和二次反应中的相对量相同。在体外免疫NIP-Ficoll后,NIP-CG引物小鼠脾片段比未免疫小鼠脾片段产生更多的IgG抗nip抗体。然而,当这些片段被同源抗原NIP-CG攻击时,IgG的数量要高得多。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Immunological memory after priming with a thymus independent antigen, NIP-ficoll. 4-hydroxy-5-iodo-3-nitrophenylacetyl coupled to polymer of sucrose and epichlorhydrin.
The capacity of mouse spleen fragments to mount an anti-NIP (4-hydroxy-5-iodo-3-nitrophenylacetyl) response in vitro was studied. The fragments came from unprimed, NIP-Ficoll (polymer of sucrose and epichlorhydrin) or NIP-CG (chicken globulin) primed mice. Unprimed spleen fragments from C57BL/6 mice gave a good anti-NIP response to NIP-Ficoll, whereas CBA fragments did not. Priming with NIP-Ficoll made CBA fragments responsive and enhanced slightly the response of C57BL/6 fragments when stimulated with the same antigen. This memory effect could be seen only after a small priming dose. Priming the mice with NIP-Ficoll made their spleen fragments responsive to a protein conjugate of NIP (NIP-CG), but this effect was seen only after priming with a high dose. The antibody class distribution and the kinetics of the appearance of different immunoglobulin classes were similar in the primary and secondary responses in vitro. The peak responses of IgM, IgA and IgG were reached on day eight and the relative amount of IgG was the same in the primary and in the secondary responses. Spleen fragments derived from NIP-CG primed mice produced more IgG anti-NIP antibodies than fragments derived from untreated mice when immunized in vitro with NIP-Ficoll. The amount of IgG was, however, much higher when these fragments were challenged with the homologous antigen, NIP-CG.
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