Cinnamaldehyde hydrazone derivatives as potential cathepsin B inhibitors: parallel in-vitro investigation in liver and cerebrospinal fluid

化学 组织蛋白酶B 肉桂醛 IC50型 体外 组织蛋白酶 脑脊液 药理学 姜黄素 对接(动物) 生物信息学 组织蛋白酶D 生物化学 立体化学 生物 医学 病理 催化作用 护理部 基因
作者
Chanchal Vashisth,Tushar Kaushik,Naman Vashisth,Neera Raghav
出处
期刊:International Journal of Biological Macromolecules [Elsevier BV]
卷期号:272 (Pt 1): 132684-132684 被引量:7
标识
DOI:10.1016/j.ijbiomac.2024.132684
摘要

The emergence of cathepsins as a potential target for anticancer drugs has led to extensive research in the development of their inhibitors. In the present study, we designed, synthesized, and characterized several cinnamaldehyde schiff bases employing diverse hydrazines, as potential cathepsin B inhibitors. The parallel studies on cathepsin B isolated from liver and cerebrospinal fluid unveiled the significance of the synthesized compounds as cathepsin B inhibitors at nanomolar concentrations. The compound, 7 exhibited the highest inhibition of 83.48 % and 82.96 % with an IC50 value of 0.06 nM and 0.09 nM for liver and cerebrospinal fluid respectively. The inhibitory potential of synthesized compounds has been extremely effective in comparison to previous reports. With the help of molecular docking studies using iGEMDOCK software, we found that the active site -CH2SH group is involved in the case of α-N-benzoyl-D, l-arginine-b-naphthylamide (BANA), curcumin 2, 3, 6, and 7. For toxicity prediction, ADMET studies were conducted and the synthesized compounds emerged to be non-toxic. The results obtained from the in vitro studies were supported with in silico studies. The synthesized cinnamaldehyde schiff bases can be considered promising drug candidates in conditions with elevated cathepsin B levels.
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