Analogues of Oxamate, Pyruvate, and Lactate as potential inhibitors of Plasmodium Knowlesi lactate Dehydrogenase identified using virtual screening and verified via Inhibition Assays

Malaria management remains a challenge, due to the resistance of malaria parasites to current antimalarial agents. This resistance consequently delays the global elimination of malaria throughout the world. Hence, the demand is increasing for new and effective antimalarial drugs. The identificati...

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Main Authors: Ahmad Fuad, Fazia Adyani, Ogu Salim, Nurhainis
Format: Article
Language:English
Published: Multidisciplinary Digital Publishing Institute (MDPI) 2022
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Online Access:http://irep.iium.edu.my/102173/1/102173_Analogues%20of%20Oxamate%2C%20Pyruvate%2C%20and%20Lactate.pdf
http://irep.iium.edu.my/102173/
https://www.mdpi.com/2227-9717/10/11/2443
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Institution: Universiti Islam Antarabangsa Malaysia
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spelling my.iium.irep.1021732022-12-29T04:17:00Z http://irep.iium.edu.my/102173/ Analogues of Oxamate, Pyruvate, and Lactate as potential inhibitors of Plasmodium Knowlesi lactate Dehydrogenase identified using virtual screening and verified via Inhibition Assays Ahmad Fuad, Fazia Adyani Ogu Salim, Nurhainis Q Science (General) QD Chemistry Malaria management remains a challenge, due to the resistance of malaria parasites to current antimalarial agents. This resistance consequently delays the global elimination of malaria throughout the world. Hence, the demand is increasing for new and effective antimalarial drugs. The identification of potential drugs that target Pk-LDH can be obtained through virtual screening analyses, as this has been previously applied to discover Pf-LDH inhibitors. In this study, the selected candidates from our virtual screening analyses were subsequently tested against purified Pk-LDH, and verified through an inhibition of Pk-LDH via enzymatic activity assays. Virtual screening analysis from this study showed that 3,3-Difluoropyrrolidine hydrochloride and 3-hydroxytetrahydrofuran exhibited binding affinity values of −3.25 kcal/mol and −3.74, respectively. These compounds were selected for evaluation towards inhibitory activity against Pk-LDH assays, including two compounds from a previous study which are oxalic acid and glycolamide. The earlier compounds were structurally similar to lactate and pyruvate, and the latter two compounds were structurally similar to a known LDH inhibitor, oxamate. Among all of the compounds tested, oxalic acid showed the highest inhibition activity at 54.12%; interestingly, this correlated well with the virtual screening analyses, which showed that this compound was the best among the Oxamate analogues, with a binding affinity value of −2.59 kcal/mol. Hence, further exploration and development of this compound may result in a promising antimalarial drug for malaria treatment, especially for infection involving P. Knowlesi. Multidisciplinary Digital Publishing Institute (MDPI) 2022-11-18 Article PeerReviewed application/pdf en http://irep.iium.edu.my/102173/1/102173_Analogues%20of%20Oxamate%2C%20Pyruvate%2C%20and%20Lactate.pdf Ahmad Fuad, Fazia Adyani and Ogu Salim, Nurhainis (2022) Analogues of Oxamate, Pyruvate, and Lactate as potential inhibitors of Plasmodium Knowlesi lactate Dehydrogenase identified using virtual screening and verified via Inhibition Assays. Processes, 10 (11). pp. 1-8. ISSN 2227-9717 https://www.mdpi.com/2227-9717/10/11/2443 10.3390/pr10112443
institution Universiti Islam Antarabangsa Malaysia
building IIUM Library
collection Institutional Repository
continent Asia
country Malaysia
content_provider International Islamic University Malaysia
content_source IIUM Repository (IREP)
url_provider http://irep.iium.edu.my/
language English
topic Q Science (General)
QD Chemistry
spellingShingle Q Science (General)
QD Chemistry
Ahmad Fuad, Fazia Adyani
Ogu Salim, Nurhainis
Analogues of Oxamate, Pyruvate, and Lactate as potential inhibitors of Plasmodium Knowlesi lactate Dehydrogenase identified using virtual screening and verified via Inhibition Assays
description Malaria management remains a challenge, due to the resistance of malaria parasites to current antimalarial agents. This resistance consequently delays the global elimination of malaria throughout the world. Hence, the demand is increasing for new and effective antimalarial drugs. The identification of potential drugs that target Pk-LDH can be obtained through virtual screening analyses, as this has been previously applied to discover Pf-LDH inhibitors. In this study, the selected candidates from our virtual screening analyses were subsequently tested against purified Pk-LDH, and verified through an inhibition of Pk-LDH via enzymatic activity assays. Virtual screening analysis from this study showed that 3,3-Difluoropyrrolidine hydrochloride and 3-hydroxytetrahydrofuran exhibited binding affinity values of −3.25 kcal/mol and −3.74, respectively. These compounds were selected for evaluation towards inhibitory activity against Pk-LDH assays, including two compounds from a previous study which are oxalic acid and glycolamide. The earlier compounds were structurally similar to lactate and pyruvate, and the latter two compounds were structurally similar to a known LDH inhibitor, oxamate. Among all of the compounds tested, oxalic acid showed the highest inhibition activity at 54.12%; interestingly, this correlated well with the virtual screening analyses, which showed that this compound was the best among the Oxamate analogues, with a binding affinity value of −2.59 kcal/mol. Hence, further exploration and development of this compound may result in a promising antimalarial drug for malaria treatment, especially for infection involving P. Knowlesi.
format Article
author Ahmad Fuad, Fazia Adyani
Ogu Salim, Nurhainis
author_facet Ahmad Fuad, Fazia Adyani
Ogu Salim, Nurhainis
author_sort Ahmad Fuad, Fazia Adyani
title Analogues of Oxamate, Pyruvate, and Lactate as potential inhibitors of Plasmodium Knowlesi lactate Dehydrogenase identified using virtual screening and verified via Inhibition Assays
title_short Analogues of Oxamate, Pyruvate, and Lactate as potential inhibitors of Plasmodium Knowlesi lactate Dehydrogenase identified using virtual screening and verified via Inhibition Assays
title_full Analogues of Oxamate, Pyruvate, and Lactate as potential inhibitors of Plasmodium Knowlesi lactate Dehydrogenase identified using virtual screening and verified via Inhibition Assays
title_fullStr Analogues of Oxamate, Pyruvate, and Lactate as potential inhibitors of Plasmodium Knowlesi lactate Dehydrogenase identified using virtual screening and verified via Inhibition Assays
title_full_unstemmed Analogues of Oxamate, Pyruvate, and Lactate as potential inhibitors of Plasmodium Knowlesi lactate Dehydrogenase identified using virtual screening and verified via Inhibition Assays
title_sort analogues of oxamate, pyruvate, and lactate as potential inhibitors of plasmodium knowlesi lactate dehydrogenase identified using virtual screening and verified via inhibition assays
publisher Multidisciplinary Digital Publishing Institute (MDPI)
publishDate 2022
url http://irep.iium.edu.my/102173/1/102173_Analogues%20of%20Oxamate%2C%20Pyruvate%2C%20and%20Lactate.pdf
http://irep.iium.edu.my/102173/
https://www.mdpi.com/2227-9717/10/11/2443
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