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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Membrane and soluble Fc gamma RII/III modulate the antigen-presenting capacity of murine dendritic epidermal Langerhans cells for IgG-complexed antigens.
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Membrane and soluble Fc gamma RII/III modulate the antigen-presenting capacity of murine dendritic epidermal Langerhans cells for IgG-complexed antigens.

机译:膜和可溶性FcγRII / III调节鼠树突状表皮朗格汉斯细胞对IgG复合抗原的抗原呈递能力。

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摘要

Murine dendritic epidermal Langerhans cells (LC) are APC. This implies that LC take up, process, and present Ag to T cells. One way of doing so that could allow Ag internalization is provided by the low affinity receptors for the Fc region of IgG (Fc gamma R), which murine LC are known to express, although their isoform(s) and function(s) have not been defined. By using molecular biology and biochemical approaches, we demonstrated that LC expressed Fc gamma RIIb2 and Fc gamma RIII. Furthermore, LC internalized Fc gamma R by receptor-mediated endocytosis, as observed with gold-labeled anti-Fc gamma RII/III mAb or immune complexes. We demonstrated the biologic relevance of this process by observing that Fc gamma R-mediated Ag internalization improved by approximately 300-fold the Ag-presenting capacity of LC to T cells. Moreover, analysis of cell culture supernatants showed that two forms of soluble Fc gamma R (sFc gamma R) were released by LC: the first most probably was the secreted transmembrane-deleted Fc gamma RII isoform, Fc gamma RIIb3, and the second was a soluble receptor probably derived from the membrane-associated Fc gamma RII/III. The ability of two recombinant forms, corresponding to the two sFc gamma R released by LC, to inhibit Fc gamma R-mediated presentation enhancement was assayed. Preincubation of IgG-complexed Ag with either rsFc gamma R led to a dose-dependent decrease in the Ag-presenting capacity of LC. Taken together, our results suggest that, in vivo, LC express membrane Fc gamma R, which increase their Ag-presenting capacity for IgG-complexed Ag, and release sFc gamma R, which might be able to modulate this Ag presentation.
机译:鼠树突状表皮朗格汉斯细胞(LC)是APC。这意味着LC吸收,处理Ag并将其呈递给T细胞。 IgG Fc区的低亲和力受体(FcγR)提供了一种可能使Ag内在化的方式,虽然它们的同种型和功能没有,但已知它们会表达鼠类LC。被定义。通过使用分子生物学和生化方法,我们证明了LC表达FcγRIIb2和FcγRIII。此外,LC通过受体介导的内吞作用使FcγR内在化,如金标记的抗FcγRII / III mAb或免疫复合物所观察到的。我们通过观察FcγR介导的Ag内在化提高了LC对T细胞的Ag呈递能力的300倍,证明了该过程的生物学相关性。此外,细胞培养上清液的分析表明,LC释放了两种形式的可溶性FcγR(sF​​cγR):第一种可能是分泌的跨膜缺失的FcγRII亚型,FcγRIIb3,第二种是可溶性受体可能源自与膜相关的FcγRII / III。测定了两种重组形式(对应于LC释放的两种sFcγR)抑制FcγR介导的呈递增强的能力。 IgG复合的Ag与任一rsFcγR的预孵育导致LC的Ag呈递能力呈剂量依赖性降低。两者合计,我们的结果表明,在体内,LC表达膜FcγR,这会增加其对IgG复合Ag的Ag呈递能力,并释放sFcγR,这可能能够调节这种Ag呈递。

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