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Revealing the potency of 1,3,5-trisubstituted pyrazoline as antimalaria through combination of in silico studies

The potency of 1,3,5-trisubstituted pyrazoline as an antimalarial agent has been studied through quantitative structure-activity relationship, molecular docking, and molecular dynamics simulation as a combination of in silico studies. The study commenced by applying quantitative structure-activity r...

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Main Authors: Rasyid, Herlina, Soekamto, Nunuk Hariani, Firdausiah, Syadza, Mardiyanti, Riska, Bahrun,, Siswanto,, Aswad, Muhammad, Saputri, Wahyu Dita, Suma, Artania A. T., Nur Hilal Syahrir,, Listyarini, Risnita Vicky
Format: Article
Language:English
Published: Penerbit Universiti Kebangsaan Malaysia 2023
Online Access:http://journalarticle.ukm.my/23331/1/SS%2010.pdf
http://journalarticle.ukm.my/23331/
https://www.ukm.my/jsm/english_journals/vol52num10_2023/contentsVol52num10_2023.html
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spelling my-ukm.journal.233312024-04-03T01:16:39Z http://journalarticle.ukm.my/23331/ Revealing the potency of 1,3,5-trisubstituted pyrazoline as antimalaria through combination of in silico studies Rasyid, Herlina Soekamto, Nunuk Hariani Firdausiah, Syadza Mardiyanti, Riska Bahrun, Siswanto, Aswad, Muhammad Saputri, Wahyu Dita Suma, Artania A. T. Nur Hilal Syahrir, Listyarini, Risnita Vicky The potency of 1,3,5-trisubstituted pyrazoline as an antimalarial agent has been studied through quantitative structure-activity relationship, molecular docking, and molecular dynamics simulation as a combination of in silico studies. The study commenced by applying quantitative structure-activity relationship (QSAR) to 25 derivative compounds using 3D-descriptor. The genetic algorithm and multiple linear regression analysis were used to construct the QSAR model, which resulting an equation that has Rtraining as 0.8100 and Rtest set as 0.9222. Descriptors involved in the QSAR equation are TDB4 m, TDB8s, RDF30e, and RDF552, all of which belong to the group of 3D autocorrelation and RDF. This result is in line with the principal component analysis, which shows that both group descriptors represent whole 3D descriptors. Molecular docking analysis is conducted to study the interaction between pyrazoline derivatives and the falcipain-2 enzyme. Interactions between compound 14 and falcipain-2 is describing by hydrogen bond against Glu14 amino acid residue, more pi-stacking interaction, and van der Waals. Chloroquine as a positive control also presented one hydrogen bond with Gly83, pi-sulfur against Cys42, and van der Waals. The stability of the ligand– enzyme interaction is evaluated by molecular dynamics simulation, and after 100 ns simulations, the root mean square deviation results show that compound 14 and chloroquine have a stable interaction with the falcipain-2 enzyme. Overall, this research provides the insight of 1,3,5-trisubstitued pyrazoline compounds as antimalaria by giving a QSAR equation and used to design a better falcipain-2 inhibitors. Penerbit Universiti Kebangsaan Malaysia 2023 Article PeerReviewed application/pdf en http://journalarticle.ukm.my/23331/1/SS%2010.pdf Rasyid, Herlina and Soekamto, Nunuk Hariani and Firdausiah, Syadza and Mardiyanti, Riska and Bahrun, and Siswanto, and Aswad, Muhammad and Saputri, Wahyu Dita and Suma, Artania A. T. and Nur Hilal Syahrir, and Listyarini, Risnita Vicky (2023) Revealing the potency of 1,3,5-trisubstituted pyrazoline as antimalaria through combination of in silico studies. Sains Malaysiana, 52 (10). pp. 2855-2867. ISSN 0126-6039 https://www.ukm.my/jsm/english_journals/vol52num10_2023/contentsVol52num10_2023.html
institution Universiti Kebangsaan Malaysia
building Tun Sri Lanang Library
collection Institutional Repository
continent Asia
country Malaysia
content_provider Universiti Kebangsaan Malaysia
content_source UKM Journal Article Repository
url_provider http://journalarticle.ukm.my/
language English
description The potency of 1,3,5-trisubstituted pyrazoline as an antimalarial agent has been studied through quantitative structure-activity relationship, molecular docking, and molecular dynamics simulation as a combination of in silico studies. The study commenced by applying quantitative structure-activity relationship (QSAR) to 25 derivative compounds using 3D-descriptor. The genetic algorithm and multiple linear regression analysis were used to construct the QSAR model, which resulting an equation that has Rtraining as 0.8100 and Rtest set as 0.9222. Descriptors involved in the QSAR equation are TDB4 m, TDB8s, RDF30e, and RDF552, all of which belong to the group of 3D autocorrelation and RDF. This result is in line with the principal component analysis, which shows that both group descriptors represent whole 3D descriptors. Molecular docking analysis is conducted to study the interaction between pyrazoline derivatives and the falcipain-2 enzyme. Interactions between compound 14 and falcipain-2 is describing by hydrogen bond against Glu14 amino acid residue, more pi-stacking interaction, and van der Waals. Chloroquine as a positive control also presented one hydrogen bond with Gly83, pi-sulfur against Cys42, and van der Waals. The stability of the ligand– enzyme interaction is evaluated by molecular dynamics simulation, and after 100 ns simulations, the root mean square deviation results show that compound 14 and chloroquine have a stable interaction with the falcipain-2 enzyme. Overall, this research provides the insight of 1,3,5-trisubstitued pyrazoline compounds as antimalaria by giving a QSAR equation and used to design a better falcipain-2 inhibitors.
format Article
author Rasyid, Herlina
Soekamto, Nunuk Hariani
Firdausiah, Syadza
Mardiyanti, Riska
Bahrun,
Siswanto,
Aswad, Muhammad
Saputri, Wahyu Dita
Suma, Artania A. T.
Nur Hilal Syahrir,
Listyarini, Risnita Vicky
spellingShingle Rasyid, Herlina
Soekamto, Nunuk Hariani
Firdausiah, Syadza
Mardiyanti, Riska
Bahrun,
Siswanto,
Aswad, Muhammad
Saputri, Wahyu Dita
Suma, Artania A. T.
Nur Hilal Syahrir,
Listyarini, Risnita Vicky
Revealing the potency of 1,3,5-trisubstituted pyrazoline as antimalaria through combination of in silico studies
author_facet Rasyid, Herlina
Soekamto, Nunuk Hariani
Firdausiah, Syadza
Mardiyanti, Riska
Bahrun,
Siswanto,
Aswad, Muhammad
Saputri, Wahyu Dita
Suma, Artania A. T.
Nur Hilal Syahrir,
Listyarini, Risnita Vicky
author_sort Rasyid, Herlina
title Revealing the potency of 1,3,5-trisubstituted pyrazoline as antimalaria through combination of in silico studies
title_short Revealing the potency of 1,3,5-trisubstituted pyrazoline as antimalaria through combination of in silico studies
title_full Revealing the potency of 1,3,5-trisubstituted pyrazoline as antimalaria through combination of in silico studies
title_fullStr Revealing the potency of 1,3,5-trisubstituted pyrazoline as antimalaria through combination of in silico studies
title_full_unstemmed Revealing the potency of 1,3,5-trisubstituted pyrazoline as antimalaria through combination of in silico studies
title_sort revealing the potency of 1,3,5-trisubstituted pyrazoline as antimalaria through combination of in silico studies
publisher Penerbit Universiti Kebangsaan Malaysia
publishDate 2023
url http://journalarticle.ukm.my/23331/1/SS%2010.pdf
http://journalarticle.ukm.my/23331/
https://www.ukm.my/jsm/english_journals/vol52num10_2023/contentsVol52num10_2023.html
_version_ 1797908402060394496
score 13.188404

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