Department of Intensive Care Medicine, Radboud Center for Infectious Diseases (RCI), Radboud University Medical Center, Nijmegen, The Netherlands.
UMR 942 Inserm, University Paris Diderot, INI-CRCT, APHP, Department of Anesthesia, Burn and Critical Care, Hôpitaux Universitaire Saint Louis Lariboisière, Paris, France.
Toxicol Appl Pharmacol. 2019 Apr 15;369:1-16. doi: 10.1016/j.taap.2019.02.014. Epub 2019 Feb 27.
Adrenomedullin (ADM) is a vasoactive peptide in sepsis. The non-neutralizing ADM-binding antibody Adrecizumab improved outcome in animal models of systemic inflammation and sepsis. Herein, we evaluated the preclinical safety of Adrecizumab in various animal species. First, Wistar rats received vehicle, 100, 200 or 400 mg/kg/day of Adrecizumab intravenously (n = 20 each) on days 1, 4, 8 and 14. An additional set of rats received vehicle or 400 mg/kg/day (n = 10 each) on the same days and were followed for 42 days. For toxicokinetics, satellite animals received vehicle (n = 6), 100, 200, or 400 mg/kg/day Adrecizumab intravenously (n = 18 each). A hemodynamic study was performed in Beagle dogs (n = 3) receiving vehicle (day 1), 2 mg/kg (day 3), 10 mg/kg (day 5), 50 mg/kg (day 8) and 10 mg/kg Adrecizumab intravenously (day 29). In final experiments, cynomolgus monkeys received vehicle, 25, 50 or 100 mg/kg/day Adrecizumab intravenously (n = 6 each) on days 1, 4, 8 and 14. Additional groups of monkeys received vehicle or 100 mg/kg/day Adrecizumab intravenously (n = 4 each) on the same days and were followed for 42 days. No mortality or moribund conditions occurred and no toxicologically relevant effects were attributed to Adrecizumab. Adrecizumab significantly increased circulating concentrations of its target peptide ADM, consistent with previous studies and mechanistically relevant. Toxicokinetic analyses showed immediate and dose-dependent peak concentrations, slow elimination and no gender differences. In conclusion, intravenous, repeated administration of high doses of Adrecizumab appeared well-tolerated across species. These results pave the way for further investigation of Adrecizumab in humans (intended dose of 2 mg/kg).
肾上腺髓质素(ADM)是脓毒症中的一种血管活性肽。非中和性 ADM 结合抗体 Adrecizumab 改善了全身性炎症和脓毒症动物模型的预后。在此,我们评估了 Adrecizumab 在各种动物物种中的临床前安全性。首先,Wistar 大鼠在第 1、4、8 和 14 天分别接受静脉注射 0、100、200 或 400mg/kg/天的 Adrecizumab(每组 20 只)。另一组大鼠在相同的日子里接受 0 或 400mg/kg/天(每组 10 只),并随访 42 天。对于毒代动力学,卫星动物接受静脉注射 0(n=6)、100、200 或 400mg/kg/天的 Adrecizumab(每组 18 只)。在接受静脉注射 0(第 1 天)、2mg/kg(第 3 天)、10mg/kg(第 5 天)、50mg/kg(第 8 天)和 10mg/kg Adrecizumab(第 29 天)的比格犬中进行了一项血液动力学研究。在最后的实验中,食蟹猴接受静脉注射 0、25、50 或 100mg/kg/天的 Adrecizumab(每组 6 只),在第 1、4、8 和 14 天。另外两组食蟹猴在相同的日子里接受 0 或 100mg/kg/天的 Adrecizumab 静脉注射(每组 4 只),并随访 42 天。没有死亡或濒死情况发生,也没有将毒性相关的作用归因于 Adrecizumab。Adrecizumab 显著增加了其靶肽 ADM 的循环浓度,与之前的研究一致,且具有机制相关性。毒代动力学分析显示立即出现且剂量依赖性的峰值浓度、缓慢消除和无性别差异。总之,跨物种静脉重复给予高剂量的 Adrecizumab 似乎具有良好的耐受性。这些结果为进一步研究 Adrecizumab 在人类中的应用铺平了道路(预期剂量为 2mg/kg)。
