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B细胞亚群介导的针对半抗原的载体导向性应答。

Carrier-directed anti-hapten responses by B-cell subsets.

作者信息

Lewis G K, Goodman J W

出版信息

J Exp Med. 1977 Jul 1;146(1):1-10. doi: 10.1084/jem.146.1.1.

Abstract

The capacity of the trinitrophenyl (TNP) haptenic group, coupled to a series of chemically dissimilar carriers, to cross-stimulate putative T- dependent and T-independent murine B-cell subpepulations was determined by using an in vitro limiting dilution technique to generate primary IgM responses. It was found that TNP-Ficoll and TNP-dextran, two T- independent antigens with little or no polyclonal mitogenicity, stimulate the same population of anti-TNP precursors, which is distinct from the precursor population activated by TNP-bacterial lipopolysaccharide (LPS), a T-independent polyclonal mitogen, or TNP-horse erythrocytes (HRBC), a T-dependent antigen. On the other hand, TNP-LPS and TNP-HRBC activate the same precursor population, indicating that LPS can substitute for the T- cell signal in T-dependent B-cell responses, whereas nonmitogenic T- independent antigens cannot. However, the cumulative evidence from this and other laboratories strongly indicates that LPS and T-dependent antigens activate B cells by different mechanisms. Of particular interest, LPS is incapable of activating B cells responsive to weakly- or nonmitogenic T-independent antigens. Based on clonal burst size, T-dependent antigens are capable of inducing greater antigen-specific B-cell proliferation than T-independent antigens. However, TNP conjugates of Ficoll and dextran, which are relatively poor inducers of polyclonal B-cell activation, induced larger anti-TNP clones than did TNP-LPS, a strong polyclonal mitogen. The findings reinforce the evidence favoring existence of multiple B- cell subpopulations with distinctive activation pathways. They also strengthen the proposition that a given B-cell subset can be activated by more than one mechanism.

摘要

通过使用体外有限稀释技术来产生初次IgM反应,确定了与一系列化学性质不同的载体偶联的三硝基苯基(TNP)半抗原基团对假定的T细胞依赖性和T细胞非依赖性小鼠B细胞亚群进行交叉刺激的能力。结果发现,TNP-菲可和TNP-葡聚糖这两种几乎没有或没有多克隆促有丝分裂活性的T细胞非依赖性抗原,刺激的是同一群抗TNP前体细胞,这与由T细胞非依赖性多克隆促有丝分裂原TNP-细菌脂多糖(LPS)或T细胞依赖性抗原TNP-马红细胞(HRBC)激活的前体细胞群不同。另一方面,TNP-LPS和TNP-HRBC激活的是同一前体细胞群,这表明LPS可以在T细胞依赖性B细胞反应中替代T细胞信号,而非促有丝分裂的T细胞非依赖性抗原则不能。然而,来自本实验室和其他实验室的累积证据有力地表明,LPS和T细胞依赖性抗原通过不同机制激活B细胞。特别有趣的是,LPS无法激活对弱促有丝分裂或无促有丝分裂活性的T细胞非依赖性抗原产生反应的B细胞。基于克隆爆发大小,T细胞依赖性抗原比T细胞非依赖性抗原能够诱导更强的抗原特异性B细胞增殖。然而,菲可和葡聚糖的TNP偶联物,它们是相对较弱的多克隆B细胞激活诱导剂,却比强多克隆促有丝分裂原TNP-LPS诱导出更大的抗TNP克隆。这些发现进一步证明了存在具有独特激活途径的多个B细胞亚群。它们还强化了这样一种观点,即给定的B细胞亚群可以通过不止一种机制被激活。

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