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首页> 外文期刊>The Journal of Experomental Medicine >Antigen-dependent IgM-mediated enhancement of the sheep erythrocyte response in mice. Evidence for induction of B cells with specificities other than that of the injected antibodies
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Antigen-dependent IgM-mediated enhancement of the sheep erythrocyte response in mice. Evidence for induction of B cells with specificities other than that of the injected antibodies

机译:抗原依赖性IgM介导的小鼠绵羊红细胞应答增强。诱导B细胞具有不同于所注射抗体的特异性的证据

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Monoclonal or polyclonal IgM-anti-SRBC antibodies were used to enhance the anti-SRBC PFC response in mice. For potentiation to occur, the IgM antibodies must always be presented with the antigen for which they have specificity. No enhancement of anti-SRBC response above control levels was noted with either antibodies alone or with antibodies used together with non-cross-reacting antigens. The degree of enhancement was independent of whether only one or several different monoclonal IgM antibodies were used. Likewise, the fine specificity variation among the antibody clones failed to influence the anti- SRBC potentiation, which was shown to vary only with the amount of IgM bound to SRBC measured by hemolytic titers. The response against epitopes on the SRBC other than those the IgM recognized was also enhanced. This was determined by injecting SRBC and a monoclonal anti-SRBC IgM that did not crossreact with GRBC into mice, and measuring the response against both antigens. Normally SRBC and GRBC cross- react at the B cell level to approximately 30 percent, and in this experiment they did so both in the control group and in the IgM group. Using antigens that only cross-react significantly at the T cell level (SRBC and HRBC), IgM-antibodies would only enhance the anti-HRBC response if SRBC and HRBC were inoculated together. No anti-HRBC potentiation was noted when antibodies were injected alone or together with either SRBC or HRBC. The data indicate that the constant part of the IgM molecule is of major importance in determining its enhancing properties in acute IgM-mediated potentiation of the immune responses. No evidence was obtained for a decisive role of variable regions. Furthermore, no general B cell activating properties of either mono- or polyclonal IgM-anti-SRBC antibodies could be demonstrated.
机译:单克隆或多克隆IgM-抗SRBC抗体被用于增强小鼠的抗SRBC PFC反应。为了产生增强作用,IgM抗体必须始终与它们具有特异性的抗原一起呈递。单独的抗体或与非交叉反应抗原一起使用的抗体均未发现抗SRBC反应高于对照水平。增强程度与是否仅使用一种或几种不同的单克隆IgM抗体无关。同样,抗体克隆之间的精细特异性变化也无法影响抗SRBC的增强,这表明仅随溶血滴度测量的SRBC结合的IgM量而变化。除IgM识别的抗原决定簇外,还增强了对SRBC抗原决定簇的响应。通过将SRBC和未与GRBC交叉反应的单克隆抗SRBC IgM注射入小鼠,并测量针对这两种抗原的反应来确定。正常情况下,SRBC和GRBC在B细胞水平发生大约30%的交叉反应,在本实验中,它们在对照组和IgM组中均如此。使用仅在T细胞水平上显着交叉反应的抗原(SRBC和HRBC),如果将SRBC和HRBC一起接种,IgM抗体只会增强抗HRBC反应。单独或与SRBC或HRBC一起注射抗体时,未观察到抗HRBC增强作用。数据表明,IgM分子的恒定部分对于确定其在急性IgM介导的免疫应答增强中的增强特性至关重要。没有证据表明可变区起决定性作用。此外,没有证明单克隆或多克隆IgM-抗SRBC抗体具有一般的B细胞活化特性。

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