首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Interleukin 5 induces S mu-S gamma 1 DNA rearrangement in B cells activated with dextran-anti-IgD antibodies and interleukin 4: a three component model for Ig class switching
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Interleukin 5 induces S mu-S gamma 1 DNA rearrangement in B cells activated with dextran-anti-IgD antibodies and interleukin 4: a three component model for Ig class switching

机译:白介素5诱导葡聚糖抗IgD抗体和白介素4激活的B细胞中S mu-Sγ1 DNA重排:Ig类转换的三成分模型

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摘要

The cellular signals required for induction of immunoglobulin (Ig) class switching are only partially understood. Two processes that are considered to be necessary for such induction are DNA synthesis and germline constant heavy (CH) gene transcription. We now show that an additional signal, as mediated by interleukin 5 (IL-5), is also required. To induce proliferation of resting B cells, but not Ig secretion, we utilized anti-IgD antibodies conjugated to dextran (alpha delta-dex). The addition of IL-4, a well-established switch factor for the IgG1 subclass, to alpha delta-dex-activated cell cultures failed to induce IgG1 secretion or mIgG1+ cells unless IL-5 was also present. While IL-4 stimulated an increase in germline gamma 1 RNA in alpha delta-dex-activated cells, this effect could neither be induced nor enhanced by IL-5. By contrast, IL-5 strongly enhanced steady-state levels of productive gamma 1 RNA induced by alpha delta-dex and IL-4, suggesting that IL-5 stimulated IgG1 switch rearrangement. To test this possibility we measured switch (S) mu-S gamma 1 DNA recombination events using a newly developed assay, digestion circularization polymerase chain reaction (DC-PCR). We demonstrated that IL-5 was necessary for induction of S mu-S gamma 1 DNA rearrangement in alpha delta-dex plus IL-4-activated cells but that it had little effect on rearrangement in the absence of IL-4. Our data strongly suggest, therefore, a three-component model for induction of Ig class switching. This model includes germline CH gene transcription, DNA synthesis, and a third component that is necessary for recombination.
机译:诱导免疫球蛋白(Ig)类别转换所需的细胞信号仅被部分理解。被认为是这种诱导所必需的两个过程是DNA合成和种系恒重(CH)基因转录。我们现在显示,还需要白介素5(IL-5)介导的其他信号。为了诱导静息B细胞增殖,而不诱导Ig分泌,我们利用与葡聚糖(alpha delta-dex)偶联的抗IgD抗体。除非存在IL-5,否则将IL-4(一种针对IgG1亚类的公认的转换因子)添加到alpha delta-dex激活的细胞培养物中将无法诱导IgG1分泌或mIgG1 +细胞。尽管IL-4刺激了由alphaδ-dex激活的细胞中种系gamma 1 RNA的增加,但IL-5既不能诱导也不能增强这种作用。相比之下,IL-5强烈增强了由alpha delta-dex和IL-4诱导的生产性γ1RNA的稳态水平,表明IL-5刺激了IgG1开关的重排。为了测试这种可能性,我们使用新开发的测定法-消化环化聚合酶链反应(DC-PCR)测量了开关(S)mu-S gamma 1 DNA重组事件。我们证明了IL-5是诱导αdelta-dex加IL-4激活的细胞中S mu-Sγ1 DNA重排所必需的,但是在没有IL-4的情况下,它对重排几乎没有影响。因此,我们的数据有力地提出了诱导Ig类转换的三成分模型。该模型包括种系CH基因转录,DNA合成和重组所需的第三种成分。

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