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Synthesis of Novel Benzimidazole Analogs for Neurodegenerative Diseases by Targeting Prolyl Oligopeptidase

Abdul Shakoor, Aftab Alam, Mumtaz Ali, Naeem Ullah, Sobia Ahsan Halim, Munir Ur Rehman, Abdullah F. Alasmari, Fawaz Alasmari, Ajmal Khan, Momin Khan, Ahmed Al‐Harrasi

2024ChemistrySelect20 citationsDOIOpen Access PDF

Abstract

Abstract A novel series of benzimidazole hydrazone‐Schiff bases have been prepared through multi‐step reaction process and structurally confirmed by 13 C‐, 1 H‐NMR and HR‐MS (ESI) spectroscopic techniques and evaluated against prolyl oligopeptidase (POP) inhibitory activity. In the series, eleven derivatives 20 , 14 15 , 19 , 10 , 9 , 11 , 4 , 5 , 18 , and 21 revealed excellent inhibition potential having IC 50 values from (IC 50 =1.44±0.08 μM) to (IC 50 =5.66±0.48 μM). However, six out of twenty compounds 12, 16, 13, 17, 22 , and 3 attributed significant activity while, three compounds were found good active in the range of IC 50 values 10.43±0.57 to 11.45±0.63 μM. The docking studies indicates that the hydrazone moiety show an imperative part in binding with one of the catalytic residues (Arg643) in the substrate binding region of POP enzyme. The excellent inhibitions of these compounds for POP enzyme may lead them to be a good candidates for drug against neurodegenerative diseases.

Topics & Concepts

OligopeptidaseBenzimidazoleMoietyChemistryStereochemistryDocking (animal)HydrazoneEnzymeActive siteBenzothiazoleLead compoundCombinatorial chemistryBiochemistryIn vitroOrganic chemistryMedicineNursingPeptidase Inhibition and AnalysisNeuropeptides and Animal PhysiologyPneumocystis jirovecii pneumonia detection and treatment