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Using an in vitro xenoantibody-mediated complement-dependent cytotoxicity model to evaluate the complement inhibitory activity of the peptidic C3 inhibitor Cp40

机译:使用体外异种抗体介导的补体依赖性细胞毒性模型评估肽C3抑制剂Cp40的补体抑制活性

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摘要

Simple and reliable methods for evaluating the inhibitory effects of drug candidates on complement activation are essential for preclinical development. Here, using an immortalized porcine aortic endothelial cell line (iPEC) as target, we evaluated the feasibility and effectiveness of an in vitro xenoantibody-mediated complement-dependent cytotoxicity (CDC) model for evaluating the complement inhibitory activity of Cp40, a potent analog of the peptidic C3 inhibitor compstatin. The binding of human xenoantibodies to iPECs led to serum dilution-dependent cell death. Pretreatment of the human serum with Cp40 almost completely inhibited the deposition of C3 fragments and C5b-9 on the cells, resulting in a dose-dependent inhibition of CDC against the iPECs. Using the same method to compare the effects of Cp40 on complement activation in humans, rhesus and cynomolgus monkeys, we found that the inhibitory patterns were similar overall. Thus, the in vitro xenoantibody-mediated CDC assay may have considerable potential for future clinical use. (C) 2015 Elsevier Inc. All rights reserved.
机译:评估候选药物对补体激活抑制作用的简单可靠方法对于临床前开发至关重要。在这里,我们使用永生化的猪主动脉内皮细胞系(iPEC)作为靶标,评估了体外异种抗体介导的补体依赖性细胞毒性(CDC)模型用于评估Cp40的补体抑制活性的可行性和有效性。肽类C3抑制剂坎普他汀。人异种抗体与iPEC的结合导致血清稀释依赖性细胞死亡。用Cp40预处理人血清几乎完全抑制了C3片段和C5b-9在细胞上的沉积,从而导致CDC对iPEC的剂量依赖性抑制。使用相同的方法比较Cp40对人类,恒河猴和食蟹猴的补体激活的影响,我们发现总体上抑制模式相似。因此,体外异种抗体介导的CDC分析可能具有未来临床应用的巨大潜力。 (C)2015 Elsevier Inc.保留所有权利。

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