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长期使用 PI3K p110α 抑制剂会导致抗氧化剂含量出现性别和组织依赖性变化,但不会影响线粒体功能。

Prolonged treatment with a PI3K p110α inhibitor causes sex- and tissue-dependent changes in antioxidant content, but does not affect mitochondrial function.

机构信息

Discipline of Nutrition, School of Medical Sciences, University of Auckland, Auckland, New Zealand.

Maurice Wilkins Centre for Molecular Biodiscovery, University of Auckland, Auckland, New Zealand.

出版信息

Biosci Rep. 2020 Oct 30;40(10). doi: 10.1042/BSR20201128.

DOI:10.1042/BSR20201128
PMID:33006363
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7569204/
Abstract

Genetic inhibition of the p110α isoform of phosphatidylinositol-3-kinase (PI3K) can increase murine lifespan, enhance mitochondrial function and alter tissue-specific oxidative balance. Here, we investigated whether pharmacological inhibition of the p110α isoform of PI3K induces similar enhancement of mitochondrial function in middle-aged mice. Eight-month-old male and female mice were fed a diet containing 0.3 g/kg of the p110α-selective inhibitor BYL-719 (BYL) or a vehicle diet (VEH) for 6 weeks. Mice consuming BYL-719 had higher blood glucose and insulin, and tended towards decreased body weight. After 72 h, gene expression of the mitochondrial biogenesis mediators Pgc1α, Tfam and Nrf1 was greater in liver of BYL-719 males only, but unchanged in skeletal muscle of either sex. Six weeks of BYL-719 treatment did not affect mitochondrial content or function in the liver or skeletal muscle of either sex. In livers of males only, the expression of the antioxidant genes Nfe2l2, Cat, Sod1 and Sod2 increased within 72 h of BYL-719 treatment, and remained higher after 6 weeks. This was associated with an increase in hepatic GSH content and catalase protein expression, and lower H2O2 levels. Our results suggest that pharmacological inhibition of p110α in adult mice does not affect liver or skeletal muscle mitochondrial function, but does show sex- and tissue-specific effects on up-regulation of antioxidant response.

摘要

基因抑制磷脂酰肌醇-3-激酶(PI3K)的 p110α 同工型可以延长小鼠的寿命,增强线粒体功能并改变组织特异性氧化平衡。在这里,我们研究了是否药理学抑制 PI3K 的 p110α 同工型会在中年小鼠中引起类似的线粒体功能增强。将 8 个月大的雄性和雌性小鼠用含有 0.3 g/kg p110α 选择性抑制剂 BYL-719(BYL)或载体饮食(VEH)的饮食喂养 6 周。食用 BYL-719 的小鼠血糖和胰岛素升高,体重有下降趋势。72 小时后,雄性小鼠肝脏中与线粒体生物发生相关的介质 Pgc1α、Tfam 和 Nrf1 的基因表达更高,但雌性小鼠的骨骼肌中没有变化。六周的 BYL-719 治疗并未影响肝脏或骨骼肌中任何性别动物的线粒体含量或功能。仅在雄性小鼠的肝脏中,抗氧化基因 Nfe2l2、Cat、Sod1 和 Sod2 的表达在 BYL-719 处理后的 72 小时内增加,并在 6 周后仍保持较高水平。这与肝 GSH 含量和过氧化氢酶蛋白表达的增加以及 H2O2 水平的降低有关。我们的结果表明,成年小鼠中 p110α 的药理学抑制不会影响肝脏或骨骼肌的线粒体功能,但确实表现出性别和组织特异性的抗氧化反应上调作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/12fb/7569204/318d2d432427/bsr-40-bsr20201128-g10.jpg
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