Moon Sun Jin, Dong Wentao, Stephanopoulos Gregory N, Sikes Hadley D
Department of Chemical Engineering Massachusetts Institute of Technology Cambridge Massachusetts USA.
Bioeng Transl Med. 2020 Sep 8;5(3):e10184. doi: 10.1002/btm2.10184. eCollection 2020 Sep.
Mitochondrial NADPH protects cells against mitochondrial oxidative stress by serving as an electron donor to antioxidant defense systems. However, due to technical challenges, it still remains unknown as to the pool size of mitochondrial NADPH, its dynamics, and NADPH/NADP ratio. Here, we have systemically modulated production rates of HO in mitochondria and assessed mitochondrial NADPH metabolism using iNap sensors, C glucose isotopic tracers, and a mathematical model. Using sensors, we observed decreases in mitochondrial NADPH caused by excessive generation of mitochondrial HO, whereas the cytosolic NADPH was maintained upon perturbation. We further quantified the extent of mitochondrial NADPH/NADP based on the mathematical analysis. Utilizing C glucose isotopic tracers, we found increased activity in the pentose phosphate pathway (PPP) accompanied small decreases in the mitochondrial NADPH pool, whereas larger decreases induced both PPP activity and glucose anaplerosis. Thus, our integrative and quantitative approach provides insight into mitochondrial NADPH metabolism during mitochondrial oxidative stress.
线粒体NADPH作为抗氧化防御系统的电子供体,保护细胞免受线粒体氧化应激的影响。然而,由于技术挑战,线粒体NADPH的库大小、其动态变化以及NADPH/NADP比率仍然未知。在这里,我们系统地调节了线粒体中HO的产生速率,并使用iNap传感器、C葡萄糖同位素示踪剂和数学模型评估了线粒体NADPH代谢。使用传感器,我们观察到线粒体HO的过度产生导致线粒体NADPH减少,而在受到干扰时细胞质NADPH保持不变。我们进一步基于数学分析量化了线粒体NADPH/NADP的程度。利用C葡萄糖同位素示踪剂,我们发现磷酸戊糖途径(PPP)的活性增加伴随着线粒体NADPH库的小幅减少,而更大程度的减少则诱导了PPP活性和葡萄糖回补。因此,我们的综合定量方法为线粒体氧化应激期间的线粒体NADPH代谢提供了见解。
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