首页> 美国卫生研究院文献>The Journal of Experimental Medicine >B-cell tolerance. IV. Differential role of surface IgM and IgD in determining tolerance susceptibility of murine B cells
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B-cell tolerance. IV. Differential role of surface IgM and IgD in determining tolerance susceptibility of murine B cells

机译:B细胞耐受性。 IV。表面IgM和IgD在确定鼠B细胞耐受敏感性中的差异作用

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摘要

During ontogeny IgD appears later than IgM on splenocytes of neonatal mice (1) and at a time when mice develop a markedly increased immune responsiveness (2). Based on these observations, it was suggested that IgD serves as a “triggering” isotype for induction of immune responses, whereas surface IgM functions as a tolerizing receptor (3). To test this hypothesis, the susceptibility of adult splenocytes (which are predominantly μ(+)δ(+)[4-6]) and neonatal splenocytes (which bear predominantly IgM [μp(+); 1, 4-6]) to tolerance induction were compared. The results indicate that neonatal splenic B cells responsive to thymus dependent (TD) antigens are exquisitely susceptible to tolerance induction compared with those from adult mice (7-9). However, cells from both adult and neonatal mice were highly susceptible to tolerance induction when thymus independent (TI) antigen was used as immunogen (8). These results suggest that the major precursor for the TD response is a μ(+)δ(+)-cell which appears late in ontogeny and is resistant to tolerance induction and that the μp(+)-cell is the major precursor for the TI response and is highly susceptible to tolerance induction. Other differences between responders for TI and TD antigens have been described previously (10-12). To test this concept, adult splenocytes were treated with papain under conditions in which IgD, but not five other surface molecules, was removed (13). Such treated splenocytes were shown to be markedly susceptible to tolerance induction, resembling TD responders from neonatal animals. This experiment was interpreted as indicating that IgD confers resistance to tolerance induction on μ(+)δ(+)-cells. To prove this interpretation, it is necessary to show that specific removal of IgD with anti-δ also results in increased susceptibility to tolerance induction and that treatment with anti-μ does not have a similar effect. In the present studies, we have removed surface IgM or IgD by antibody-induced capping and assessed the tolerance susceptibility of the treated cells. Our results demonstrate that removal of IgD, but no IgM, from TD responders increases their susceptibility to tolerance induction.
机译:在个体发育过程中,新生小鼠脾细胞中IgD的出现要晚于IgM(1),而小鼠的免疫应答显着增加(2)。基于这些观察结果,有人建议IgD充当诱导免疫应答的“触发”同种型,而表面IgM充当耐受性受体(3)。为了验证这一假设,成人脾细胞(主要为μ(+)δ(+)[4-6])和新生儿脾细胞(主要为IgM [μp(+); 1、4-6])对比较耐受诱导。结果表明,与成年小鼠相比,对胸腺依赖性(TD)抗原有反应的新生儿脾B细胞对耐受诱导非常敏感(7-9)。但是,当使用胸腺独立(TI)抗原作为免疫原时,成年和新生小鼠的细胞都极易诱导耐受耐受(8)。这些结果表明,TD反应的主要前体是μ(+)δ(+)细胞,该细胞出现在个体发育后期,并且对耐受诱导具有抗性,而μp(+)细胞是TI的主要前体。响应,并且很容易引起容忍。 TI和TD抗原的应答者之间的其他差异先前已有描述(10-12)。为了检验这一概念,在去除IgD而不去除其他五个表面分子的条件下,用木瓜蛋白酶处理成人脾细胞(13)。已显示此类处理的脾细胞对耐受诱导显着敏感,类似于新生动物的TD响应者。该实验被解释为表明IgD赋予了对μ(+)δ(+)细胞的耐受诱导的抗性。为了证明这一解释,必须证明用抗δ特异性清除IgD也会导致对耐受诱导的敏感性增加,并且用抗μ进行治疗不会产生相似的效果。在本研究中,我们通过抗体诱导的加帽去除了表面IgM或IgD,并评估了所处理细胞的耐受性。我们的结果表明,从TD应答者中除去IgD,但不除去IgM,会增加其对耐受诱导的敏感性。

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