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首页> 外文期刊>Blood cancer journal. >Anti-leukemic activity and tolerability of anti-human CD47 monoclonal antibodies
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Anti-leukemic activity and tolerability of anti-human CD47 monoclonal antibodies

机译:抗人CD47单克隆抗体的抗白血病活性和耐受性

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CD47, a broadly expressed cell surface protein, inhibits cell phagocytosis via interaction with phagocyte-expressed SIRPα. A variety of hematological malignancies demonstrate elevated CD47 expression, suggesting that CD47 may mediate immune escape. We discovered three unique CD47-SIRPα blocking anti-CD47 monoclonal antibodies (mAbs) with low nano-molar affinity to human and cynomolgus monkey CD47, and no hemagglutination and platelet aggregation activity. To characterize the anti-cancer activity elicited by blocking CD47, the mAbs were cloned into effector function silent and competent Fc backbones. Effector function competent mAbs demonstrated potent activity in vitro and in vivo, while effector function silent mAbs demonstrated minimal activity, indicating that blocking CD47 only leads to a therapeutic effect in the presence of Fc effector function. A non-human primate study revealed that the effector function competent mAb IgG1 C47B222-(CHO) decreased red blood cells (RBC), hematocrit and hemoglobin by >40% at 1?mg/kg, whereas the effector function silent mAb IgG2σ C47B222-(CHO) had minimal impact on RBC indices at 1 and 10?mg/kg. Taken together, our findings suggest that targeting CD47 is an attractive therapeutic anti-cancer approach. However, the anti-cancer activity observed with anti-CD47 mAbs is Fc effector dependent as are the side effects observed on RBC indices.
机译:CD47是一种广泛表达的细胞表面蛋白,可通过与吞噬细胞表达的SIRPα相互作用来抑制细胞吞噬作用。多种血液系统恶性肿瘤显示CD47表达升高,提示CD47可能介导免疫逃逸。我们发现了三种独特的CD47-SIRPα阻断性抗CD47单克隆抗体(mAb),它们与人和食蟹猴CD47的纳摩尔摩尔亲和力低,并且无血凝和血小板聚集活性。为了表征通过阻断CD47引发的抗癌活性,将单克隆抗体克隆到效应功能沉默的和有能力的Fc骨架中。效应功能感受态mAb在体外和体内均表现出有效的活性,而效应功能沉默的mAb表现出最小的活性,表明在存在Fc效应功能的情况下,阻断CD47仅可导致治疗作用。一项非人类灵长类动物研究显示,效应器功能胜任的mAb IgG1 C47B222-(CHO)在1?mg / kg时可使红细胞(RBC),血细胞比容和血红蛋白降低40%以上,而效应器功能沉默的mAbIgG2σC47B222- (CHO)对RBC指数(1和10?mg / kg)的影响最小。综上所述,我们的发现表明靶向CD47是一种有吸引力的治疗性抗癌方法。但是,用抗CD47 mAb观察到的抗癌活性是Fc效应子依赖性的,正如在RBC指数上观察到的副作用一样。

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