Neutrophil activation in response to immune complex-bearing endothelial cells depends on the functional cooperation of Fc gamma RII (CD32) and Fc gamma RIII (CD16).

R Moser, H Etter, L Oligati, J Fehr
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Abstract

Leukoclastic vasculitis is thought to be initiated by deposition of immune complexes (ICs) in the vascular wall. To study the neutrophil response in a related in vitro model, we primed human umbilical vein endothelial cell (HUVEC) monolayers with antibodies against human fibronectin. The resulting respiratory burst to the immobilized ICs depended on the antibody concentration used to prime the monolayers and included a marked release of primary and secondary granule constituents. On IC-bearing HUVEC monolayers, but not on ICs directly bound to tissue culture dishes, blocking monoclonal antibodies (mAbs) to crystallizable fragment-gamma receptor II (Fc gamma RII) and Fc gamma RIII markedly inhibited the respiratory burst and the release of elastase. However, on both surfaces the neutrophil response was strongly inhibited by mAbs against CD18. Regardless of whether we used neutrophils from a patient with severe paroxysmal nocturnal hemoglobinuria (PNH) lacking the Fc gamma RIII, or whether the Fc gamma RII-mediated signal transduction was blocked by pertussis toxin, the respiratory burst to the IC-bearing HUVECs was essentially unchanged. With PNH neutrophils, the respiratory burst was predominantly blocked by an anti-Fc gamma RII mAb. In contrast, the response of pertussis toxin treated neutrophils was strongly inhibited by a mAb against Fc gamma RIII. Together these data indicate that the answer of neutrophils to ICs immobilized at the endothelial barrier depends on the cooperative function of both low-affinity Fc gamma Rs.

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中性粒细胞对承载免疫复合物的内皮细胞的激活依赖于Fc γ RII (CD32)和Fc γ RIII (CD16)的功能合作。
白细胞破裂性血管炎被认为是由免疫复合物(ic)沉积在血管壁引起的。为了在相关的体外模型中研究中性粒细胞反应,我们在人脐静脉内皮细胞(HUVEC)单层中注入了抗人纤维连接蛋白的抗体。所产生的对固定化ic的呼吸爆发取决于用于引物单层的抗体浓度,并包括一次和二次颗粒成分的显著释放。在含ic的HUVEC单层上,而不是直接与组织培养液结合的ic上,阻断可结晶片段γ受体II (Fc gamma RII)和Fc gamma RIII的单克隆抗体(mab)显著抑制呼吸爆发和弹性蛋白酶的释放。然而,在这两个表面上,中性粒细胞反应被CD18单克隆抗体强烈抑制。无论我们是否使用来自缺乏Fc γ RIII的严重突发性夜间血红蛋白尿(PNH)患者的中性粒细胞,或者Fc γ rii介导的信号转导是否被百日咳毒素阻断,对含ic的HUVECs的呼吸爆发基本不变。对于PNH中性粒细胞,呼吸爆发主要被抗fc γ RII单抗阻断。相比之下,百日咳毒素处理的中性粒细胞的反应被针对Fc γ RIII的单抗强烈抑制。这些数据表明,中性粒细胞对固定在内皮屏障上的ic的反应取决于低亲和力Fc γ Rs的协同功能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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