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抑制性B细胞因子对抗体形成的反馈调节:记忆B淋巴细胞对高亲和力抗体产生的优先抑制

Feedback regulation of antibody formation by suppressive B cell factor: preferential suppression of high-affinity antibody production by memory B lymphocytes.

作者信息

Park Y H, Suzuki T, Miyama-Inaba M, Masuda T, Yoshida Y, Uchino H

出版信息

Int Arch Allergy Appl Immunol. 1986;81(2):156-64. doi: 10.1159/000234125.

Abstract

Cloned TS4.44 cells, which were hybridized HAT-sensitive 3T3-4E cells with B cells stimulated by immune complexes produce a lymphokine, biochemical and biological characteristics of which are identical with those of conventional suppressive B cell factor (SBF) synthesized by Fc receptor bearing B cells stimulated with immune complexes. This factor is known to suppress B cell responses to antigen/mitogen. The present studies were carried out by using this hybridoma-derived SBF to characterize the large proportion of B cells sensitive to SBF and the small proportion of B cells resistant to it in terms of affinities of antibodies which these cells are able to produce. The treatment of normal spleen cells with SBF resulted in a 50-70% decrease in anti-dinitrophenyl (DNP) antibody production when the cells were transferred into X-ray-irradiated mice along with alum-precipitated dinitrophenyl-conjugated keyhole limpet hemocyanin (DNP-KLH). The affinity of anti-DNP antibody molecules produced in these mice was significantly lower than that of the controls, even if immunization was repeated. The target cells for SBF were B, and not helper T cells which might be involved in the process of affinity maturation. A single treatment of spleen cells in vitro with SBF was sufficient to abrogate the precursors committed to mediate high-affinity anti-DNP antibody responses, since the retreatment with SBF in vitro and transfer into the second irradiated recipients along with antigens of spleen cells of mice to which SBF-treated spleen cells were transferred 3 weeks before resulted in almost the same level of plaque-forming-cell-responses as in mice which received medium-treated.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

克隆的TS4.44细胞是由对HAT敏感的3T3 - 4E细胞与经免疫复合物刺激的B细胞杂交产生的,它能产生一种淋巴因子,其生化和生物学特性与由携带Fc受体的B细胞经免疫复合物刺激合成的传统抑制性B细胞因子(SBF)相同。已知该因子可抑制B细胞对抗原/有丝分裂原的反应。本研究利用这种杂交瘤来源的SBF,根据这些细胞能够产生的抗体亲和力,来表征对SBF敏感的大部分B细胞和对其有抗性的小部分B细胞。当将正常脾细胞与明矾沉淀的二硝基苯基结合的血蓝蛋白(DNP - KLH)一起转移到经X射线照射的小鼠体内时,用SBF处理正常脾细胞会导致抗二硝基苯基(DNP)抗体产生减少50 - 70%。即使重复免疫,这些小鼠产生的抗DNP抗体分子的亲和力也明显低于对照组。SBF的靶细胞是B细胞,而不是可能参与亲和力成熟过程的辅助性T细胞。在体外对脾细胞进行单次SBF处理就足以消除致力于介导高亲和力抗DNP抗体反应的前体细胞,因为在体外再次用SBF处理并与3周前接受过SBF处理的脾细胞的小鼠的脾细胞抗原一起转移到第二组经照射的受体小鼠体内,所产生的空斑形成细胞反应水平与接受培养基处理的小鼠几乎相同。(摘要截短至250字)

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