第一次给药OKT3后出现双相粒细胞减少。

F J Bemelman, S Buysmann, S L Yong, F N van Diepen, P T Schellekens, R J ten Berge
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引用次数: 0

摘要

在第一次给药后5小时,比较了第二种免疫球蛋白G2a (IgG2a)抗cd3单克隆抗体(mAb) OKT3及其同型开关变体IgA对粒细胞动力学的影响。此外,我们还对这些单克隆抗体诱导CD11b和CD62L表达的改变进行了体内和体外研究。在给药后15分钟内,OKT3和IgG2a抗cd3单抗诱导循环粒细胞显著减少,而IgA抗cd3单抗则没有。显然,循环粒细胞最初的减少取决于给药的抗cd3单抗的重链,导致肺中的免疫细胞粘附和隔离。通过改变CD11b和CD62L的表达增加对肺内皮的粘附在第一次粒细胞减少中起次要作用,因为每种单抗在体外对这些粘附分子具有相同的作用。第二次粒细胞计数下降发生在给药后60分钟,这与体内CD11b和CD62L表达显著增加以及体外CD11b上调和CD62L下调有关。这些改变可能与体内和体外肿瘤坏死因子- α的存在有关。因此,给药后30分钟的粒细胞动力学类似于tnf - α诱导的中性粒细胞动力学。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Biphasic granulocytopenia after administration of the first dose of OKT3.

The effects of the administration of OKT3, a second immunoglobulin G2a (IgG2a) anti-CD3 monoclonal antibody (mAb), and its isotype switch variant IgA on granulocyte kinetics were compared for 5 hours after the first administration of the mAb. In addition, in vivo and in vitro studies were performed on alterations in expression of CD11b and CD62L induced by these mAbs. Within 15 minutes after administration OKT3 and IgG2a anti-CD3 mAbs induced a significant decrease in circulating granulocytes, whereas IgA anti-CD3 mAb did not. Apparently the initial decrease in circulating granulocytes depends on the heavy chain of the administered anti-CD3 mAb, resulting in immunocytoadherence and sequestration in the lungs. Increased adherence to pulmonary endothelium by altered expression of CD11b and CD62L plays a minor role in this first granulocytopenia, because each mAb exerted the same effects on these adhesion molecules in vitro. The second decrease in granulocyte counts occurred 60 minutes after administration of each mAb and correlated with a significant increase in expression of CD11b and CD62L in vivo and with upregulation of CD11b and down-regulation of CD62L in vitro. These alterations could be related to the presence of tumor necrosis factor-alpha both in vivo and in vitro. Thus granulocyte kinetics from 30 minutes after administration of each anti-CD3 mAb resemble neutrophil kinetics induced by TNF-alpha.

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