Genomic and non-genomic regulation of PGC1 isoforms by estrogen to increase cerebral vascular mitochondrial biogenesis and reactive oxygen species protection

Martin F. Kemper; Chris Stirone; Diana N. Krause; Sue P. Duckies; Vincent Procaccio

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Genomic and non-genomic regulation of PGC1 isoforms by estrogen to increase cerebral vascular mitochondrial biogenesis and reactive oxygen species protection

机译：雌激素对PGC1亚型的基因组和非基因组调节，以增加脑血管线粒体的生物发生和活性氧的保护

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We previously found that estrogen exerts a novel protective effect on mitochondria in brain vasculature. Here we demonstrate in rat cerebral blood vessels that 17p-estradiol (estrogen), both in vivo and ex vivo, affects key transcriptional coactivators responsible for mitochondrial regulation. Treatment of ovariecto-mized rats with estrogen in vivo lowered mRNA levels of peroxisome proliferator-activated receptor-gamma coactivator-1 alpha (PGC-1alpha) but increased levels of the other PGC-1 isoforms: PGC-1beta and PGC-1 related coactivator (PRC). In vessels ex vivo, estrogen decreased protein levels of PGC-la via activation of phosphatidylinositol 3-kinase (PI3K). Estrogen treatment also increased phosphorylation of forkhead transcription factor, FoxOl, a known pathway for PGC-la downregulation. In contrast to the decrease in PGC-la, estrogen increased protein levels of nuclear respiratory factor 1, a known PGC target and mediator of mitochondrial biogenesis. The latter effect of estrogen was independent of PI3K, suggesting a separate mechanism consistent with increased expression of PGC-1beta and PRC. We demonstrated increased mitochondrial biogenesis following estrogen treatment in vivo; cerebrovascular levels of mitochondrial transcription factor A and electron transport chain subunits as well as the mitochondrial/ nuclear DNA ratio were increased. We examined a downstream target of PGC-1 beta, glutamate-cysteine ligase (GCL), the rate-limiting enzyme for glutathione synthesis. In vivo estrogen increased protein levels of both GCL subunits and total glutathione levels. Together these data show estrogen differentially regulates PGC-1 isoforms in brain vasculature, underscoring the importance of these coactivators in adapting mitochondria in specific tissues. By upregulating PGC-1beta and/or PRC, estrogen appears to enhance mitochondrial biogenesis, function and reactive oxygen species protection.

机译：我们先前发现雌激素对脑血管中的线粒体具有新型保护作用。在这里，我们证明了在大鼠脑血管中，体内和离体的17p-雌二醇（雌激素）都会影响负责线粒体调控的关键转录共激活因子。用雌激素在体内对卵巢切除的大鼠进行治疗可降低过氧化物酶体增殖物激活的受体-γcoactivator-1 alpha（PGC-1alpha）的mRNA水平，但增加了其他PGC-1亚型的水平：PGC-1beta和PGC-1相关的coactivator （PRC）。在离体血管中，雌激素通过激活磷脂酰肌醇3-激酶（PI3K）降低了PGC-1a的蛋白质水平。雌激素治疗还增加了叉头转录因子FoxOl的磷酸化，这是PGC-1a下调的已知途径。与PGC-1a的减少相反，雌激素增加了核呼吸因子1（一种已知的PGC靶标和线粒体生物发生的介体）的蛋白水平。雌激素的后一种作用独立于PI3K，表明与PGC-1beta和PRC表达增加一致的独立机制。我们证明体内雌激素治疗后线粒体生物发生增加;脑血管中线粒体转录因子A和电子传输链亚基的水平以及线粒体/核DNA的比例均增加。我们检查了PGC-1β的下游目标，谷氨酸-半胱氨酸连接酶（GCL），谷胱甘肽合成的限速酶。体内雌激素增加了GCL亚基和总谷胱甘肽水平的蛋白质水平。这些数据共同表明，雌激素可差异调节脑血管中的PGC-1亚型，强调了这些共激活因子在适应特定组织中线粒体中的重要性。通过上调PGC-1beta和/或PRC，雌激素似乎可以增强线粒体的生物发生，功能和活性氧的保护。

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《European Journal of Pharmacology: An International Journal》 |2014年第null期|共8页
作者
Martin F. Kemper; Chris Stirone; Diana N. Krause; Sue P. Duckies; Vincent Procaccio;
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Cerebral blood vessels; Estrogen; Glutamate-cysteine ligase; Mitochondria; Peroxisome proliferator-activated; receptor-gamma coactivator-1 (PGC-1); Glutathione;

机译：脑血管;雌激素;谷氨酸-半胱氨酸连接酶;线粒体;过氧化物酶体增殖物激活;受体-γ共激活因子-1（PGC-1）;谷胱甘肽;

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1. Genomic and non-genomic regulation of PGC1 isoforms by estrogen to increase cerebral vascular mitochondrial biogenesis and reactive oxygen species protection [J] . Martin F. Kemper, Chris Stirone, Diana N. Krause, European Journal of Pharmacology: An International Journal . 2014,第Null期

机译：雌激素对PGC1亚型的基因组和非基因组调节，以增加脑血管线粒体的生物发生和活性氧的保护
2. Oleuropein induces mitochondrial biogenesis and decreases reactive oxygen species generation in cultured avian muscle cells, possibly via an up-regulation of peroxisome proliferator-activated receptor coactivator-1 [J] . Kikusato Motoi, Muroi Hikaru, Uwabe Yuichiro, Animal Science Journal . 2016,第11期

机译：橄榄苦苷可能通过上调过氧化物酶体增殖物激活受体coactivator-1来诱导禽类肌肉细胞中线粒体的生物发生并减少活性氧的产生。
3. Redox and reactive oxygen species regulation of mitochondrial cytochrome C oxidase biogenesis [J] . BourensM., FontanesiF., SotoI.C., Antioxidants and redox signalling . 2013,第16期

机译：线粒体细胞色素C氧化酶生物合成的氧化还原和活性氧调节
4. Enhanced Generation of Mitochondrial Reactive Oxygen Species in Cybrids Containing 4977-bp Mitochondrial DNA Deletion [C] . MEI-JIE JOU, TSUNG-I PENG, HONG-YUEH WU, Asian Society for Mitochondrial Research and Medicine . 2005

机译：增强含有4977-BP线粒体DNA缺失的糖线电池活性氧物质的产生
5. Ovarian Hormones increase Mitochondrial Efficiency and Biogenesis via Distinct Regulation of PGC1 Isoforms in Cerebral Blood Vessels. [D] . Kemper, Martin Fredrick. 2012

机译：卵巢激素通过对脑血管中PGC1亚型的不同调节来提高线粒体效率和生物发生。
6. Genomic and non-genomic regulation of PGC1 isoforms by estrogen to increase cerebral vascular mitochondrial biogenesis and reactive oxygen species protection [O] . Martin F. Kemper, Chris Stirone, Diana N. Krause, -1

机译：雌激素对PGC1亚型的基因组和非基因组调节以增加脑血管线粒体的生物发生和活性氧的保护
7. Genomic and non-genomic regulation of PGC1 isoforms by estrogen to increase cerebral vascular mitochondrial biogenesis and reactive oxygen species protection [O] . M.F. Kemper, C. Stirone, D.N. Krause, 2014

机译：雌激素对pGC1同种型的基因组和非基因组调控可增加脑血管线粒体生物合成和活性氧保护

Genomic and non-genomic regulation of PGC1 isoforms by estrogen to increase cerebral vascular mitochondrial biogenesis and reactive oxygen species protection

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