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Molecular docking analysis of Omt-A protein model from with synthetic compounds. | LitMetric

Molecular docking analysis of Omt-A protein model from with synthetic compounds.

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Department of environment and forest resources, Chungnam, National University, Daehak-ro, Yuseong-gu, Daejeon, Republic of Korea.

Published: October 2023


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Article Abstract

Aflatoxin is a potent mycotoxin of Aspergillus flavus that has been classified as a Group I carcinogen. O-methyltransferase A (Omt-A) is a critical enzyme in the formation of aflatoxin. It catalyzes the methylation of norsalic acid to form the highly toxic intermediate averantin. The ligand-protein interaction of Omt-A was performed with piperlonguminin and blasticidins. The maximum affinity of -10.6 was found for the 5ICC_A piperlonguminine at site1 (X,Y,Z: -15.282, 21.785, 5.672). Compounds such as Blasticidin S, Neoeriocitrin, Blasticidin S - hydrochloric acid, 6,6''-Bigenkwanin, Pipernomaline, and Eriodictyol were found to have binding features to protein residues, as shown by computational interaction at the molecular level.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10640793PMC
http://dx.doi.org/10.6026/97320630019990DOI Listing

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