Design, synthesis, and molecular modeling of new 3(2H)-pyridazinone derivatives as acetylcholinesterase/butyrylcholinesterase inhibitors

Inhibition of cholinesterases is an effective method to curb Alzheimer’s disease, a progressive and fatal neurological disorder. A series of 6-substituted-3(2 H )-pyridazinone-2-acetyl-2-( p -substituted benzalhidrazone) derivatives were designed, synthesized, and their inhibitory effects on acetylc...

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Published inMedicinal chemistry research Vol. 26; no. 10; pp. 2293 - 2308
Main Authors Özdemir, Zeynep, Yılmaz, Hayriye, Sarı, Suat, Karakurt, Arzu, Şenol, Fatma Sezer, Uysal, Mehtap
Format Journal Article
LanguageEnglish
Published New York Springer US 01.10.2017
Springer Nature B.V
Subjects
Acetylcholinesterase
Alzheimer's disease
Biochemistry
Biomedical and Life Sciences
Biomedicine
Cell Biology
Chemical synthesis
Cholinesterase
Cholinesterase inhibitors
Derivatives
Inhibitors
Kinases
Molecular docking
Molecular modelling
Neurodegenerative diseases
Original Research
Pharmacology/Toxicology
Piperazine
Pyridazinone
BChE inhibitory
Benzalhydrazone
Pyridazinone
3
AChE inhibitory
Molecular docking
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Summary:Inhibition of cholinesterases is an effective method to curb Alzheimer’s disease, a progressive and fatal neurological disorder. A series of 6-substituted-3(2 H )-pyridazinone-2-acetyl-2-( p -substituted benzalhidrazone) derivatives were designed, synthesized, and their inhibitory effects on acetylcholinesterase and butyrylcholinesterase were evaluated in pursuit of potent dual inhibitors. We obtained our compounds by the reaction of various substituted/nonsubstituted benzaldehydes with 6-[4-(3,4-dichlorophenyl)piperazine-1-yl]-3(2 H )-pyridazinone-2-yl acetohydrazide and determined their anticholinesterase activities according to the Ellman’s method. 5f and 5i showed 75.52 and 71.72% acetylcholinesterase inhibition at 100 µg/ml, respectively. 5h and 5f , on the other hand, were the best butyrylcholinesterase inhibitors with 67.16 and 62.03% inhibition at the same concentration, respectively. 5f emerged as a potent dual cholinesterase inhibitor. Through molecular docking studies we predicted the inhibition mechanism of 5f for both enzymes in comparison with our previous derivatives, which differ in inhibition potency, and tried to get insights into the factors that affect receptor affinity in molecular level.
ISSN:1054-2523
1554-8120
DOI:10.1007/s00044-017-1930-x