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克隆无能:耐受小鼠体内存在对抗原或促有丝分裂原无反应的抗原结合B淋巴细胞。

Clonal anergy: persistence in tolerant mice of antigen-binding B lymphocytes incapable of responding to antigen or mitogen.

作者信息

Nossal G J, Pike B L

出版信息

Proc Natl Acad Sci U S A. 1980 Mar;77(3):1602-6. doi: 10.1073/pnas.77.3.1602.

Abstract

The purpose of these experiments was to determine the degree of reduction in the number of antigen-binding B lymphocytes in the spleens of mice that had been rendered tolerant in the perinatal period. Newborn or pregnant mice were injected with fluorescein (Flu) coupled onto human gamma globulin, and the spleen cells of the neonatally injected mice, or of the offspring of the pregnant mice, were analyzed 1-6 weeks later. Tolerogen doses were chosen so as to achieve either a two-thirds reduction (low dose) in the number of anti-Flu B cells capable of yielding anti-hapten plaque-forming cell clones after in vitro stimulation, or as representing a supra-optimal tolerogenic stimulus (high dose). Antigen-binding B cells were studied by a two-cycle procedure, namely an initial cycle of binding to Flu-gelatin thin layers, followed by analysis of the binding cells in the fluorescence-activated cell sorter (FACS) after suitable staining with Flu-protein conjugates. With the high dose of tolerogen, a modest diminution in Flu-binding cell numbers down to 56-71% of control values could be induced. When these residual Flu-specific B cells were analyzed in the FACS to quantitate their spectrum of Flu-binding avidities, profiles identical to those of controls were obtained. The reduction proved transient in nature, binding cell numbers having returned to 80% of normal by 2 weeks and to normal by 6 weeks. Nevertheless, the Flu-specific B cells were incapable of responding to antigen or mitogen by antibody formation. With the low dose of tolerogen, despite the desired degree of functional silencing of Flu-specific B cells, the numbers and avidity spectra of antigen-binding cells were entirely normal in both the neonatally injected and in utero-injected groups. The results indicate that tolerance induced amongst immature B lymphocytes is not due to a physical elimination of the relevant B cell clones or to a modulation or blockade of their surface Ig receptors. Rather, it is due to the recognition and storage of negative signals amongst cells that continue to display a normal complement of receptors. We therefore propose that the term "clonal anergy" is a more accurate description than either "clonal deletion" or "clonal abortion."

摘要

这些实验的目的是确定围产期诱导耐受的小鼠脾脏中抗原结合性B淋巴细胞数量减少的程度。给新生小鼠或怀孕小鼠注射与人γ球蛋白偶联的荧光素(Flu),1至6周后分析新生期注射小鼠或怀孕小鼠后代的脾细胞。选择耐受原剂量,以实现体外刺激后能够产生抗半抗原空斑形成细胞克隆的抗Flu B细胞数量减少三分之二(低剂量),或代表超最佳耐受原刺激(高剂量)。通过双循环程序研究抗原结合性B细胞,即首先与Flu-明胶薄层结合,然后在用Flu-蛋白缀合物进行适当染色后,在荧光激活细胞分选仪(FACS)中分析结合细胞。使用高剂量的耐受原,可诱导Flu结合细胞数量适度减少,降至对照值的56 - 71%。当在FACS中分析这些残留的Flu特异性B细胞以定量其Flu结合亲和力谱时,获得了与对照相同的图谱。结果证明这种减少本质上是短暂的,结合细胞数量在2周时恢复到正常的80%,6周时恢复正常。然而,Flu特异性B细胞无法通过抗体形成对抗原或有丝分裂原作出反应。使用低剂量的耐受原,尽管Flu特异性B细胞达到了预期的功能沉默程度,但在新生期注射组和子宫内注射组中,抗原结合细胞的数量和亲和力谱均完全正常。结果表明,在未成熟B淋巴细胞中诱导的耐受不是由于相关B细胞克隆的物理清除,也不是由于其表面Ig受体的调节或阻断。相反,它是由于在继续显示正常受体补体的细胞中识别和储存了负信号。因此,我们提出“克隆无能”一词比“克隆清除”或“克隆流产”更准确地描述了这种现象。

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