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Effect of B-cell receptor engagement on CD40-stimulated B cells.

机译:B细胞受体参与对CD40刺激的B细胞的影响。

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摘要

Activation of human B cells in vitro either by cross-linking of surface immunoglobulins (sIg) or by triggering CD40 antigen, in the presence of interleukin-10 (IL-10) and interleukin-2 (IL-2), may result in high levels of immunoglobulin secretion in vitro. We studied the combined effects of ligation of the B-cell receptor (BCR) and CD40 [with anti-CD40 monoclonal antibody (mAb)] on B-cell proliferation and production of human immunoglobulin. For this purpose highly purified splenic B cells were cultured with various combinations of anti-CD40 and IL-10/IL-2 or IL-4 in the presence of CD32-transfected L cells. Simultaneous cross-linking of the BCR was achieved by mAb held on CD32-L cells or Staphylococcus aureus (SA). We found that dual BCR and CD40 ligation with IL-10/IL-2 leads to reduced immunoglobulin G (IgG) secretion compared with B cells stimulated with either anti-CD40 and IL-10/IL-2, or compared with B cells stimulated with SA or anti-BCR mAb and IL-10/IL-2. Dual BCR and CD40 ligation with anti-immunoglobulin mAb (anti-kappa + anti-lambda light chains) but not with SA induced a similar reduction in IgM production. The reduced immunoglobulin secretion found during dual ligation is accompanied by increased proliferation. This was independent of cytokine stimulation but SA/CD40-induced proliferation was increased in the presence of IL-10/IL-2, although not with IL-4. The combination anti-kappa and anti-lambda with anti-CD40 showed a long-term suppression of IgG and IgM production (at least 14 days), while anti-kappa or anti-lambda alone, or SA, allowed a moderate recovery of immunoglobulin production by day 14. These results suggest that simultaneous B-cell antigen receptor cross-linking and CD40 engagement via CD40L on T cells induces strong initial proliferation. This may be followed later by antibody production depending on the strength of the BCR signal and the presence of the appropriate cytokines.
机译:在存在白介素10(IL-10)和白介素2(IL-2)的情况下,通过表面免疫球蛋白(sIg)的交联或触发CD40抗原在体外激活人B细胞,可能导致高免疫球蛋白的体外分泌水平。我们研究了B细胞受体(BCR)和CD40 [与抗CD40单克隆抗体(mAb)的连接]对B细胞增殖和人类免疫球蛋白产生的联合作用。为此目的,在CD32转染的L细胞的存在下,将高纯度的脾脏B细胞与抗CD40和IL-10 / IL-2或IL-4的各种组合一起培养。 BCR的同时交联是通过CD32-L细胞或金黄色葡萄球菌(SA)上的单克隆抗体实现的。我们发现,与用抗CD40和IL-10 / IL-2刺激的B细胞相比,或与受刺激的B细胞相比,双重BCR和CD40与IL-10 / IL-2的连接导致免疫球蛋白G(IgG)分泌减少。 SA或抗BCR mAb和IL-10 / IL-2。 BCR和CD40与抗免疫球蛋白mAb(抗κ+抗lambda轻链)的双重连接,但与SA无关,导致了IgM产量的类似降低。在双重连接过程中发现免疫球蛋白分泌减少,伴随着增殖增加。这与细胞因子刺激无关,但是在IL-10 / IL-2存在下SA / CD40诱导的增殖增加,尽管IL-4并非如此。抗-kappa和抗-lambda与抗-CD40的组合显示出对IgG和IgM产生的长期抑制作用(至少14天),而单​​独的抗-kappa或抗-lambda或SA可使免疫球蛋白适度恢复这些结果表明,在14天前同时发生B细胞抗原受体交联和CD40经由CD40L在T细胞上的结合诱导了强烈的初始增殖。随后可以根据BCR信号的强度和适当细胞因子的存在而产生抗体。

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