Zhu Jin, Jiang Xue, Li Zongzheng, Liu Shuxian, Han Jinmeng, Li Shu, Liu Ziyuan, Zhuang Tao, Zhang Guisen
Jiangsu Key Laboratory of Marine Pharmaceutical Compound Screening, School of Pharmacy, Jiangsu Ocean University, Lianyungang 222005, China.
Jiangsu Key Laboratory of Marine Pharmaceutical Compound Screening, School of Pharmacy, Jiangsu Ocean University, Lianyungang 222005, China.
Bioorg Chem. 2025 Jan;154:107997. doi: 10.1016/j.bioorg.2024.107997. Epub 2024 Nov 26.
Intravenous anesthetics play a crucial role during surgery. Etomidate, a commonly used intravenous anesthetic agent, is prized for its rapid onset and smooth induction of anesthesia. However, it has a pronounced adverse effect on adrenal function suppression. To obtain new rapid recovery hypnotic agents without adrenocortical suppression, a series of thioetomidate derivatives (TET-1-TET-14) were designed and synthesized. Among them, TET-13 (half-live T = 0.48 min) was metabolized much faster than that of etomidate (T = 26 min) in rat plasma. In rodents, TET-13 exhibited potent anesthetic effects in both mice (ED = 0.48 mg/kg) and rats (ED = 0.69 mg/kg) and demonstrated a markedly shorter recovery time compared to etomidate. In the GABAR binding assay, TET-13 acted as a positive allosteric modulator on the GABA receptor and showed an EC of 5.65 μM which was lower than etomidate (EC = 9.29 μM). At equivalent doses, TET-13 group showed significantly less adrenocortical suppression than etomidate. Moreover, in the continuous infusion test, the time to behavioral recovery and time to walk after infusion with TET-13 were all shorter than etomidate. Thioetomidate derivatives represent a promising strategy to develop new rapid recovery hypnotic agents without adrenocortical suppression.
