Exploring Novel Pyridine Carboxamide Derivatives as Urease Inhibitors: Synthesis, Molecular Docking, Kinetic Studies and ADME Profile

Ayesha Naseer; Faisal Abdulrhman Osra; Asia Naz Awan; Aqeel Imran; Abdul Hameed; Syed Adnan Ali Shah; Jamshed Iqbal; Zainul Amiruddin Zakaria

doi:10.3390/ph15101288

Pharmaceuticals (Oct 2022)

Exploring Novel Pyridine Carboxamide Derivatives as Urease Inhibitors: Synthesis, Molecular Docking, Kinetic Studies and ADME Profile

Ayesha Naseer,
Faisal Abdulrhman Osra,
Asia Naz Awan,
Aqeel Imran,
Abdul Hameed,
Syed Adnan Ali Shah,
Jamshed Iqbal,
Zainul Amiruddin Zakaria

Affiliations

Ayesha Naseer: Research Institute of Pharmaceutical Sciences, University of Karachi, Karachi 75270, Pakistan
Faisal Abdulrhman Osra: Department of Civil Engineering, Umm Al Qura University, Makkah 21961, Saudi Arabia
Asia Naz Awan: Research Institute of Pharmaceutical Sciences, University of Karachi, Karachi 75270, Pakistan
Aqeel Imran: Center for Advanced Drug Research, COMSATS University Islamabad, Abbottabad Campus, Abbottabad 22060, Pakistan
Abdul Hameed: Department of Chemistry, University of Sahiwal, Sahiwal 57000, Pakistan
Syed Adnan Ali Shah: Faculty of Pharmacy, Universiti Teknologi MARA Cawangan Selangor Kampus Puncak Alam, Bandar Puncak Alam 42300, Selangor, Malaysia
Jamshed Iqbal: Center for Advanced Drug Research, COMSATS University Islamabad, Abbottabad Campus, Abbottabad 22060, Pakistan
Zainul Amiruddin Zakaria: Borneo Research on Algesia Inflammation and Neurodegeneration (BRAIN) Group, Faculty of Medicine and Health Sciences, University Malaysia Sabah, Jalan UMS, Kota Kinabalu 88400, Sabah, Malaysia

DOI: https://doi.org/10.3390/ph15101288
Journal volume & issue: Vol. 15, no. 10
p. 1288

Abstract

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The rapid development of resistance by ureolytic bacteria which are involved in various life-threatening conditions such as gastric and duodenal cancer has induced the need to develop a new line of therapy which has anti-urease activity. A series of pyridine carboxamide and carbothioamide derivatives which also have some novel structures were synthesized via condensation reaction and investigated against urease for their inhibitory action. Among the series, 5-chloropyridine-2 yl-methylene hydrazine carbothioamide (Rx-6) and pyridine 2-yl-methylene hydrazine carboxamide (Rx-7) IC50 = 1.07 ± 0.043 µM, 2.18 ± 0.058 µM both possessed significant activity. Furthermore, molecular docking and kinetic studies were performed for the most potent inhibitors to demonstrate the binding mode of the active pyridine carbothioamide with the enzyme urease and its mode of interaction. The ADME profile also showed that all the synthesized molecules present oral bioavailability and high GI absorption.

Published in Pharmaceuticals

ISSN: 1424-8247 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine: Pharmacy and materia medica
Website: http://www.mdpi.com/journal/pharmaceuticals/

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