4.5 Article

Methionine Sources Differently Affect Production of Reactive Oxygen Species, Mitochondrial Bioenergetics, and Growth of Murine and Quail Myoblasts In Vitro

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CURRENT ISSUES IN MOLECULAR BIOLOGY
卷 45, 期 4, 页码 2661-2680

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MDPI
DOI: 10.3390/cimb45040174

关键词

methionine; HMTBA; muscle; growth; satellite cell; metabolic rate; viability; ROS

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Optimal supply of L-methionine promotes muscle growth, whereas over-supplementation has adverse effects. This study examines the effects of different methionine supplements on cell growth, viability, ROS production, and mitochondrial bioenergetics in mouse and quail myoblasts. Results show that all supplements stimulate cell growth, but high levels of L-methionine or DL-2-hydroxy-4-(methylthio)butanoic acid (DL-HMTBA) retard growth and increase extracellular H2O2 levels, indicating oxidative stress. DL-HMTBA oversupplementation also leads to adaptive changes in mitochondrial functionality. Quail cells are better able to cope with methionine oversupplementation than mouse cells.
An optimal supply of L-methionine (L-Met) improves muscle growth, whereas over-supplementation exerts adverse effects. To understand the underlying mechanisms, this study aims at exploring effects on the growth, viability, ROS production, and mitochondrial bioenergetics of C2C12 (mouse) and QM7 (quail) myoblasts additionally supplemented (100 or 1000 mu M) with L-Met, DL-methionine (DL-Met), or DL-2-hydroxy-4-(methylthio)butanoic acid (DL-HMTBA). In both cell lines, all the supplements stimulated cell growth. However, in contrast to DL-Met, 1000 mu M of L-Met (C2C12 cells only) or DL-HMTBA started to retard growth. This negative effect was stronger with DL-HMTBA and was accompanied by significantly elevated levels of extracellular H2O2, an indicator for OS, in both cell types. In addition, oversupplementation with DL-HMTBA (1000 mu M) induced adaptive responses in mitochondrial bioenergetics, including reductions in basal (C2C12 and QM7) and ATP-synthase-linked (C2C12) oxygen consumption, maximal respiration rate, and reserve capacity (QM7). Only QM7 cells switched to nonmitochondrial aerobic glycolysis to reduce ROS production. In conclusion, we found a general negative effect of methionine oversupplementation on cell proliferation. However, only DL-HMTBA-induced growth retardation was associated with OS and adaptive, species-specific alterations in mitochondrial functionality. OS could be better compensated by quail cells, highlighting the role of species differences in the ability to cope with methionine oversupplementation.

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