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In vivo and in vitro study of the primary and secondary antibody response to a bacterial antigen in aged mice.

机译:体内和体外研究老年小鼠对细菌抗原的一抗和二抗的反应。

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摘要

One of the most important manifestations of aging in both humans and laboratory animals is a gradual decline in immune effectiveness. However, it is not clear as to how general is this decline. We here report that aged BALB/c mice showed no decline in the magnitude of the in vivo primary antibody response to phosphorylcholine (PC), an immunodominant epitope of the Streptococcus pneumoniae R36a (Pn). Often it appeared that aged mice responded better than young syngeneic mice. In contrast, the secondary antibody response had a different profile, with aged mice showing a marked decrease in PC-specific antibody. Further in vitro studies were conducted in order to determine the cause of the decline of the secondary antibody response in aging. We noted that B cells from young and aged donors, either primed or twice immunized with the antigen, when cultured without T cells and in the presence of antigen did not display any significant difference in their antibody response to PC. However, L3T4 cells from aged BALB/c mice, previously immunized twice with Pn, failed to augment the in vitro B cell response as compared to L3T4 cells from young mice. Moreover, we found that Lyt 2 cells from young and aged mice had no regulatory effects on the anti-PC response in vitro. Further in vivo experiments demonstrated that alteration of the idiotypic network may not be related to a decline in the secondary antibody response since two injections of the antigen are unable to elicit an anti-idiotypic antibody response in either young or aged mice. These data demonstrate that the decline of the anti-PC response after a secondary challenge with Pn is linked to defects in the T cell compartment.
机译:人类和实验动物衰老的最重要表现之一是免疫效力的逐渐下降。但是,尚不清楚这种下降有多普遍。我们在此报告,年老的BALB / c小鼠体内对磷酰胆碱(PC)(肺炎链球菌R36a(Pn)的免疫优势表位)的体内一抗反应程度没有下降。通常看来,老年小鼠比年轻的同系小鼠反应更好。相比之下,第二抗体反应具有不同的特征,老年小鼠的PC特异性抗体明显降低。为了确定衰老中第二抗体应答下降的原因,进行了进一步的体外研究。我们注意到,在没有T细胞且存在抗原的情况下培养时,来自年轻和老年供体的B细胞(无论是用抗原引发还是免疫两次)在其对PC的抗体反应中均未显示任何显着差异。但是,与来自年轻小鼠的L3T4细胞相比,以前用Pn免疫两次的老年BALB / c小鼠的L3T4细胞未能增强体外B细胞应答。此外,我们发现来自年轻和老年小鼠的Lyt 2细胞对体外抗PC反应没有调节作用。进一步的体内实验表明,由于两次注射抗原均不能在年轻或老年小鼠中引起抗独特型抗体应答,因此独特型网络的改变可能与第二抗体应答的下降无关。这些数据表明,在用Pn进行第二次攻击后,抗PC反应的下降与T细胞区室的缺陷有关。

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