Longo D M, Generaux G T, Howell B A, Siler S Q, Antoine D J, Button D, Caggiano A, Eisen A, Iaci J, Stanulis R, Parry T, Mosedale M, Watkins P B
DILIsym Services Inc., Research Triangle Park, North Carolina, USA.
MRC Centre for Drug Safety Science, Department of Molecular & Clinical Pharmacology, Liverpool University, Liverpool, UK.
Clin Pharmacol Ther. 2017 Dec;102(6):961-969. doi: 10.1002/cpt.711. Epub 2017 May 27.
Cimaglermin alfa (GGF2) is a recombinant human protein growth factor in development for heart failure. Phase I trials were suspended when two cimaglermin alfa-treated subjects experienced concomitant elevations in serum aminotransferases and total bilirubin, meeting current US Food and Drug Administration criteria for a serious liver safety signal (i.e., "Hy's Law"). We assayed mechanistic biomarkers in archived clinical trial serum samples which confirmed the hepatic origin of the aminotransferase elevations in these two subjects and identified apoptosis as the major mode of hepatocyte death. Using a mathematical model of drug-induced liver injury (DILIsym) and a simulated population, we estimated that the maximum hepatocyte loss in these two subjects was <13%, which would not result in liver dysfunction sufficient to significantly increase serum bilirubin levels. We conclude that the two subjects should not be considered Hy's Law cases and that mechanistic biomarkers and modeling can aid in refining liver safety risk assessment in clinical trials.
西马格列明α(GGF2)是一种正在研发用于治疗心力衰竭的重组人蛋白生长因子。当两名接受西马格列明α治疗的受试者血清转氨酶和总胆红素同时升高,符合美国食品药品监督管理局目前关于严重肝脏安全信号的标准(即“海氏法则”)时,一期试验暂停。我们对存档的临床试验血清样本中的机制生物标志物进行了检测,证实了这两名受试者转氨酶升高的肝脏来源,并确定细胞凋亡是肝细胞死亡的主要方式。使用药物性肝损伤数学模型(DILIsym)和模拟人群,我们估计这两名受试者的最大肝细胞损失<13%,这不会导致足以显著提高血清胆红素水平的肝功能障碍。我们得出结论,这两名受试者不应被视为海氏法则病例,并且机制生物标志物和建模有助于在临床试验中完善肝脏安全风险评估。
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