Depletion of L‑Methionine in Foods with an Engineered Thermophilic Methionine γ‑lyase Efficiently Inhibits Tumor Growth

Dietary restriction of l-methionine, an essential amino acid, exerts potent antitumor effects on l-methionine-dependent cancers. However, dietary restriction of l-methionine has not been practical for human therapy because of the problem with the administration of l-methionine concentration in foods...

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Veröffentlicht in:Journal of agricultural and food chemistry 2023-11, Vol.71 (45), p.17141-17152
Hauptverfasser: Hu, Yangming, Liu, Yan, Zhang, Jiulin, Zhou, Zhijing, Wang, Jiaxue, Chen, Hongyang, Huang, Meina, Hu, Han, Dai, Zongjie, Jia, Kaizhi
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Sprache:eng
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Zusammenfassung:Dietary restriction of l-methionine, an essential amino acid, exerts potent antitumor effects on l-methionine-dependent cancers. However, dietary restriction of l-methionine has not been practical for human therapy because of the problem with the administration of l-methionine concentration in foods. Here, a thermophilic methionine γ-lyase (MGL), that catalyzes the cleavage of the C–S bond in l-methionine to produce α-ketobutyric acid, methanethiol, and ammonia was engineered from human cystathionine γ-lyase and almost completely depleted l-methionine at 65 °C, a temperature that accelerates the volatilization of methanethiol and its oxidation products. The high efficiency of l-methionine lysis may be attributed to the cooperative fluctuation and moderate the structural rigidity of 4 monomers in the thermophilic MGL, which facilitates l-methionine access to the entrance of the active site. Experimental diets treated with thermophilic MGL markedly inhibited prostate tumor growth in mice, and in parallel, the in vivo concentrations of l-methionine, its transformation product l-cysteine, and the oxidative stress indicator malondialdehyde significantly decreased. These findings provide a technology for the depletion of l-methionine in foods with an engineered thermophilic MGL, which efficiently inhibits tumor growth in mice.
ISSN:0021-8561
1520-5118
DOI:10.1021/acs.jafc.3c05293