在治疗诱导的低白蛋白血症和急性胰腺炎的交叉点猖獗的蛋白水解

4open Pub Date : 2022-01-01 DOI:10.1051/fopen/2022011
Sarah-Ellen Leonard, P. Kenis, Ray C. Perkins
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引用次数: 1

摘要

蛋白酶抑制是药物在多种疾病中的预期作用机制:癌症、心血管和中风、糖尿病、黄斑变性和阿尔茨海默氏症。真菌和多种病毒感染(包括Sars-Cov-2)的治疗也依赖于抑制病原体特异性蛋白酶。这项工作考察了一种此类药物奈非那韦(商品名VIRACEPT™)的非治疗性蛋白水解活性,奈非那韦被批准为HIV蛋白酶抑制剂,这是有史以来最大的“生物技术发布”。方法描述在合著的手稿中[Leonard et al. (2022), 4open 5,11]。这些方法不仅适用于靶上活性的检测,也适用于靶外活性的检测。在这里,它被证明奈非那韦作为一种抑制剂和促进关键血液蛋白的蛋白质水解活性。观察结果很容易与已知的药物诱导急性胰腺炎和伴随的低白蛋白血症联系起来。扩大分子水平,早期,脱靶/脱底物活性候选药物评估的好处变得明显。最后,药物诱发疾病的现实对现有的临床程序提出了新的要求,即将副作用视为诱发疾病的症状。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Rampant proteolysis at the intersection of therapy-induced hypoalbuminemia and acute pancreatitis
Protease inhibition is the intended mechanism of action for drugs across a broad range of diseases: cancer, cardiovascular and stroke, diabetes mellitus, macular degeneration and Alzheimer’s. Treatment for fungal and multiple viral infections, including Sars-Cov-2, also relies upon inhibition of pathogen-specific proteases. This work examines the non-therapeutic proteolytic activity of one such drug, nelfinavir (tradename VIRACEPT™), approved as an inhibitor of HIV protease, the largest, “biotech launch” in history at the time of its introduction. Methods are described in the companion manuscript [Leonard et al. (2022), 4open 5, 11]. These methods are not only suitable for examination of on-target activity but also of off-target activity. Herein, it is demonstrated that nelfinavir is active both as an inhibitor and as a promoter of proteolysis of key blood proteins. Observations are readily connected to known drug induction of acute pancreatitis and attendant hypoalbuminemia. The benefits of expanding molecular-level, early-stage, off-target/off-substrate activity drug candidate evaluation become apparent. Finally, the reality of drug-induced disease places new demands on existing clinical procedures, namely that side effects be approached as symptoms of an induced disease.
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