4.6 Article

Inhibition of Escherichia coli nitroreductase by the constituents in Syzygium aromaticum

Journal

CHINESE JOURNAL OF NATURAL MEDICINES
Volume 20, Issue 7, Pages 506-517

Publisher

CHINESE JOURNAL NATURAL MEDICINES
DOI: 10.1016/S1875-5364(22)60163-8

Keywords

Gut bacterial nitroreductase; EcNfsA inhibitor; Syzygium aromaticum; Anti-mutagenic activity

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This study found that clove extract has strong inhibitory activity against EcNfsA, and some constituents in cloves such as ellagic acid showed strong to moderate inhibitory effects, which provides a new potential pathway for reducing the toxicity induced by bacterial nitroreductase.
Gut bacterial nitroreductases play an important role in reduction of various nitroaromatic compounds to the corresponding N-nitroso compounds, hydroxylamines or aromatic amines, most of which are carcinogenic and mutagenic agents. Inhibition of gut nitroreductases has been recognized as an attractive approach for reducing mutagen metabolites in the colon, so as to prevent colon diseases. In this study, the inhibitory effects of 55 herbal medicines against Escherichia coli (E. coli) nitroreductase (EcNfsA) were examined. Compared with other herbal extracts, Syzygium aromaticum extract showed superior inhibitory potency toward EcNfsA mediated nitrofurazone reduction. Then, the inhibitory effects of 22 major constituents in Syzygium aromaticum against EcNfsA were evaluted. Compared with other tested natural compounds, ellagic acid, corilagin, betulinic acid, oleanic acid, ursolic acid, urolithin M5 and isorhamnetin were found with strong to moderate inhibitory effect against EcNfsA, with IC50 values ranging from 0.67 to 28.98 mol center dot L-1. Furthermore, the inhibition kinetic analysis and docking simulation demonstrated that ellagic acid and betulinic acid potently inhibited EcNfsA (K-i < 2 mu mol center dot L-1) in a competitively inhibitory manner, which created strong interactions with the catalytic triad of EcNfsA. In summary, our findings provide new scientific basis for explaining the anti-mutagenic activity of Syzygium aromaticum, where some newly identified EcNfsA inhibitors can be used for developing novel agents to reduce the toxicity induced by bacterial nitroreductase.

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