CD40 mAb G28-5的激动性和拮抗性取决于其结合价。

Circulatory shock Pub Date : 1994-10-01
J A Ledbetter, L S Grosmaire, D Hollenbaugh, A Aruffo, S G Nadler
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引用次数: 0

摘要

结合mAb G28-5可触发CD40功能应答。在这里,我们发现G28-5诱导部分CD40反应,并通过阻止gp39的结合,作为天然CD40配体gp39的部分拮抗剂。G28-5的Fab片段保留了抑制活性,但失去了依赖交联的刺激活性。CD40信号与PMA或CD20的协同作用显示出对CD40交联的不同要求和对环孢素A的不同敏感性,这表明CD40受体可能使用不同的效应机制与钙依赖性CD20信号或来自PMA的钙非依赖性信号协同作用。NF-kappa B在RAJI细胞中被G28-5或gp39激活,并且依赖于CD40交联。这些结果表明nf - κ B的激活参与了一些CD40受体信号,并可能与CD40刺激或抑制细胞凋亡的作用有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Agonistic and antagonistic properties of CD40 mAb G28-5 are dependent on binding valency.

CD40 functional responses can be triggered by binding of mAb G28-5. Here we show that G28-5 induces partial CD40 responses and functions as a partial antagonist of natural CD40 ligand, gp39, by preventing gp39 binding. Fab fragments of G28-5 retain inhibitory activity but lose crosslinking-dependent stimulatory activity. The synergistic interaction of CD40 signals with PMA or CD20 show differential requirements for CD40 crosslinking and different sensitivity to cyclosporine A, suggesting that CD40 receptor may use different effector mechanisms for synergy with calcium-dependent CD20 signals or with calcium-independent signals from PMA. Activation of NF-kappa B occurred in RAJI cells by G28-5 or by gp39 treatment, and was CD40 crosslinking-dependent. These results suggest that activation of NF-kappa B is involved in some CD40 receptor signals and may be related to CD40 effects on stimulation or inhibition of apotosis.

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