Multi-step synthesis, kinetics and in silico explorations of indole-Phenyl-1,2,4-triazole Bi-heterocyclic hybrids unified with 3-substituted benzamides as elastase inhibitors

Multi-step synthesis, kinetics and in silico explorations of indole-Phenyl-1,2,4-triazole Bi-heterocyclic hybrids unified with 3-substituted benzamides as elastase inhibitors

In the present research work, a library of unique indole-phenyltriazole hybrids comprising 3-substituted-benzamide moiety was synthesized through convergent multi-step strategy. The structural confirmation of all synthesized molecules was corroborated by IR, 1H NMR, 13C MMR, EI-MS and CHN analysis d...

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Published in:JOURNAL OF MOLECULAR STRUCTURE
Main Authors: Shakila; Abbasi, Muhammad Athar; Aziz-ur-Rehman; Siddiqui, Sabahat Zahra; Nazir, Majid; Muhammad, Shabbir; Raza, Hussain; Shah, Syed Adnan Ali; Shahid, Muhammad; Chaudhry, Aijaz Rasool; Kim, Song Ja
Format: Article
Language:English
Published: ELSEVIER 2025
Subjects:
Chemistry
Online Access:https://www-webofscience-com.uitm.idm.oclc.org/wos/woscc/full-record/WOS:001334908300001
author Shakila; Abbasi
Muhammad Athar; Aziz-ur-Rehman; Siddiqui
Sabahat Zahra; Nazir
Majid; Muhammad
Shabbir; Raza
Hussain; Shah
Syed Adnan Ali; Shahid
Muhammad; Chaudhry
Aijaz Rasool; Kim
Song Ja
spellingShingle Shakila; Abbasi
Muhammad Athar; Aziz-ur-Rehman; Siddiqui
Sabahat Zahra; Nazir
Majid; Muhammad
Shabbir; Raza
Hussain; Shah
Syed Adnan Ali; Shahid
Muhammad; Chaudhry
Aijaz Rasool; Kim
Song Ja
Multi-step synthesis, kinetics and in silico explorations of indole-Phenyl-1,2,4-triazole Bi-heterocyclic hybrids unified with 3-substituted benzamides as elastase inhibitors
Chemistry
author_facet Shakila; Abbasi
Muhammad Athar; Aziz-ur-Rehman; Siddiqui
Sabahat Zahra; Nazir
Majid; Muhammad
Shabbir; Raza
Hussain; Shah
Syed Adnan Ali; Shahid
Muhammad; Chaudhry
Aijaz Rasool; Kim
Song Ja
author_sort Shakila; Abbasi
spelling Shakila; Abbasi, Muhammad Athar; Aziz-ur-Rehman; Siddiqui, Sabahat Zahra; Nazir, Majid; Muhammad, Shabbir; Raza, Hussain; Shah, Syed Adnan Ali; Shahid, Muhammad; Chaudhry, Aijaz Rasool; Kim, Song Ja
Multi-step synthesis, kinetics and in silico explorations of indole-Phenyl-1,2,4-triazole Bi-heterocyclic hybrids unified with 3-substituted benzamides as elastase inhibitors
JOURNAL OF MOLECULAR STRUCTURE
English
Article
In the present research work, a library of unique indole-phenyltriazole hybrids comprising 3-substituted-benzamide moiety was synthesized through convergent multi-step strategy. The structural confirmation of all synthesized molecules was corroborated by IR, 1H NMR, 13C MMR, EI-MS and CHN analysis data. The results of in vitro inhibitory potential of novel benzamides against elastase enzyme revealed that all molecules were potent inhibitors and 10d was most active compound among them having IC50 value of (0.197 +/- 0.027 mu M), relative to the standard (13.421 +/- 0.016 mu M). The Kinetics mechanism analyzed by Lineweaver-Burk plots which exposed that 10d inhibited this enzyme competitively by forming an enzyme-inhibitor complex. The inhibition constant Ki determined from Dixon plot for compound 10d was 0.85 mu M. Moreover, cytotoxicity of these compounds was also profiled by hemolytic activity and it was observed that almost all these benzamides compounds displayed low cytotoxicity. These molecules also exhibited mild cytotoxicity toward red blood cell membrane. In addition, the in silico computational explorations fully supported the in vitro enzyme inhibitory results. The binding energy ranges from -7.1 to -9.1 kcal/mol, which showed that compound possessed good interaction tendencies to the pancreatic elastase target protein. So, it was anticipated from the experimental results and computational investigations of the current research that these derivatives might lead to further research gateways for obtaining better and safe nontoxic medicinal scaffolds for dealing with the elastase related ailments such as lungs diseases, pruritic skin disease and liver infection.
ELSEVIER
0022-2860
1872-8014
2025
1322

10.1016/j.molstruc.2024.140192
Chemistry

WOS:001334908300001
https://www-webofscience-com.uitm.idm.oclc.org/wos/woscc/full-record/WOS:001334908300001
title Multi-step synthesis, kinetics and in silico explorations of indole-Phenyl-1,2,4-triazole Bi-heterocyclic hybrids unified with 3-substituted benzamides as elastase inhibitors
title_short Multi-step synthesis, kinetics and in silico explorations of indole-Phenyl-1,2,4-triazole Bi-heterocyclic hybrids unified with 3-substituted benzamides as elastase inhibitors
title_full Multi-step synthesis, kinetics and in silico explorations of indole-Phenyl-1,2,4-triazole Bi-heterocyclic hybrids unified with 3-substituted benzamides as elastase inhibitors
title_fullStr Multi-step synthesis, kinetics and in silico explorations of indole-Phenyl-1,2,4-triazole Bi-heterocyclic hybrids unified with 3-substituted benzamides as elastase inhibitors
title_full_unstemmed Multi-step synthesis, kinetics and in silico explorations of indole-Phenyl-1,2,4-triazole Bi-heterocyclic hybrids unified with 3-substituted benzamides as elastase inhibitors
title_sort Multi-step synthesis, kinetics and in silico explorations of indole-Phenyl-1,2,4-triazole Bi-heterocyclic hybrids unified with 3-substituted benzamides as elastase inhibitors
container_title JOURNAL OF MOLECULAR STRUCTURE
language English
format Article
description In the present research work, a library of unique indole-phenyltriazole hybrids comprising 3-substituted-benzamide moiety was synthesized through convergent multi-step strategy. The structural confirmation of all synthesized molecules was corroborated by IR, 1H NMR, 13C MMR, EI-MS and CHN analysis data. The results of in vitro inhibitory potential of novel benzamides against elastase enzyme revealed that all molecules were potent inhibitors and 10d was most active compound among them having IC50 value of (0.197 +/- 0.027 mu M), relative to the standard (13.421 +/- 0.016 mu M). The Kinetics mechanism analyzed by Lineweaver-Burk plots which exposed that 10d inhibited this enzyme competitively by forming an enzyme-inhibitor complex. The inhibition constant Ki determined from Dixon plot for compound 10d was 0.85 mu M. Moreover, cytotoxicity of these compounds was also profiled by hemolytic activity and it was observed that almost all these benzamides compounds displayed low cytotoxicity. These molecules also exhibited mild cytotoxicity toward red blood cell membrane. In addition, the in silico computational explorations fully supported the in vitro enzyme inhibitory results. The binding energy ranges from -7.1 to -9.1 kcal/mol, which showed that compound possessed good interaction tendencies to the pancreatic elastase target protein. So, it was anticipated from the experimental results and computational investigations of the current research that these derivatives might lead to further research gateways for obtaining better and safe nontoxic medicinal scaffolds for dealing with the elastase related ailments such as lungs diseases, pruritic skin disease and liver infection.
publisher ELSEVIER
issn 0022-2860
1872-8014
publishDate 2025
container_volume 1322
container_issue
doi_str_mv 10.1016/j.molstruc.2024.140192
topic Chemistry
topic_facet Chemistry
accesstype
id WOS:001334908300001
url https://www-webofscience-com.uitm.idm.oclc.org/wos/woscc/full-record/WOS:001334908300001
record_format wos
collection Web of Science (WoS)
_version_ 1814778545260462080

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