Toxicology profile of a novel GLP1 receptor biased agonist-SAL0112 in nonhuman primates

兴奋剂 受体 生物 非人灵长类 计算生物学 进化生物学 遗传学
作者
Jingchao Sun,Yao Xiao,Xuefeng Hu,Shuqing Chen,Jing Huang,Zhiqiang Ren,Binbin Luo,Rongzhi Jiang,Hongmei Zhang,Xiaolei Shen
出处
期刊:Toxicology and Applied Pharmacology [Elsevier]
卷期号:: 117125-117125
标识
DOI:10.1016/j.taap.2024.117125
摘要

Oral small-molecule GLP-1 receptor biased agonists exhibit promising treatment efficacy of type 2 diabetes and obesity. SAL0112 is a novel compound that has demonstrated remarkable efficacy in preclinical animal models. Herein, both in vitro and in vivo preclinical toxicity investigations were conducted to explore the safety profile of SAL0112. The HTRF assay and TR-FRET assay were utilized for cAMP detection. Patch clamp assay was employed for hERG potassium ion channel determination. Cynomolgus monkeys were used in a cardiovascular safety pharmacology study and a 13-week repeated dose toxicity study. The telemetry system was employed to detect cardiovascular indicators such as ECG, HR, and BP. During the repeated dose toxicity study, body weight, food intake, hematology, coagulation function test, serum biochemistry tests, and urine analysis were measured. Macroscopic and microscopic observations were conducted at the end of the study. TK studies were conducted on Day 1 and Day 91. SAL0112 exhibited a high degree of potency in activating the monkey GLP1 receptor whereas had no effect on the rodent GLP1 receptor. In contrast to Danuglipron, which demonstrated high potency on hERG with an IC
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