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首页> 外文期刊>Redox Biology >Sinapine, but not sinapic acid, counteracts mitochondrial oxidative stress in cardiomyocytes
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Sinapine, but not sinapic acid, counteracts mitochondrial oxidative stress in cardiomyocytes

机译:辛滨,但不是辛酸,抵消了心肌细胞的线粒体氧化胁迫

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Introduction When confronted to stress or pathological conditions, the mitochondria overproduce reactive species that participate in the cellular dysfunction. These organelles are however difficult to target with antioxidants. A feature of mitochondria that can be used for this is the negatively charged compartments they form. Most of mitochondrion-targeting antioxidants are therefore cationic synthetic molecules. Our hypothesis is that such mitochondriotropic traits might also exists in natural molecules. Aim We tested here whether sinapine, a natural phenolic antioxidant-bearing a permanent positive charge, can target mitochondria to modulate mitochondrial oxidative stress. Methods Experiments were performed in-vitro , in-cellulo , ex-vivo, and in-vivo, using cardiac tissue. The sinapic acid -lacking the positively-charged-choline-moiety present in sinapine-was used as a control. Sinapine entry into mitochondria was investigated in-vivo and in cardiomyocytes. We used fluorescent probes to detect cytosolic (Hsub2/subDCFDA) and mitochondrial (DHRsub123/sub) oxidative stress on cardiomyocytes induced with either hydrogen peroxide (Hsub2/subOsub2/sub) or antimycin A, respectively. Finally, ROS production was measured with DHE 10?min after ischemia-reperfusion (IR) on isolated heart, treated or not with sinapine, sinapic acid or with a known synthetic mitochondrion-targeted antioxidant (mitoTempo). Results We detected the presence of sinapine within mitochondria in-vitro, after incubation of isolated cardiomyocytes, and in-vivo, after oral treatment. The presence of sinapic acid was not detected in the mitochondria. Both the sinapine and the sinapic acid limited cytosolic oxidative stress in response to Hsub2/subOsub2/sub. Only sinapine was able to blunt oxidative stress resulting from antimycin A-induced mtROS. Both mitoTempo and sinapine improved cardiac functional recovery following IR. This was associated with lower ROS production within the cardiac tissue. Conclusion Sinapine, a natural cationic hydrophilic phenol, commonly and substantially found in rapeseed species, effectively (i) enters within the mitochondria, (ii) selectively decreases the level of mitochondrial oxidative stress and, (iii) efficiently limits ROS production during cardiac ischemia-reperfusion.
机译:引言面对应力或病理条件时,线粒体过量的反应性物种参与细胞功能障碍。然而,这些细胞器难以靶向抗氧化剂。可以使用的线粒体的特征是它们形成的带负电的隔间。因此,大多数线粒体靶向抗氧化剂是阳离子合成分子。我们的假设是这种线粒体ropic特征也可能存在于天然分子中。目的我们在这里测试锡汀是否是一种天然酚醛抗氧化剂的永久性阳性电荷,可以靶向线粒体以调节线粒体氧化应激。方法使用心脏组织在体外,细胞内,前体内和体内进行实验。钛酸酸 - 将存在于锡滨的带正电荷的胆碱部分 - 用作对照。在体内和心肌细胞中研究了锡鞘进入线粒体。我们使用荧光探针检测用过氧化氢诱导的心肌细胞(H 2 123)和线粒体(dhr 123 )氧化应激(H 2 o 2 )或抗霉素a。最后,在脱血素 - 再灌注(IR)的缺血再灌注(IR)后,用Sinapine,SINAPIC酸或已知的合成线粒体靶向抗氧化剂(Mitotempo),用DHE 10?MIN测量ROS生产。结果在口服处理后,在体外,在体外,在体外,在体外,检测到锡汀的存在。在线粒体中未检测到锡酸的存在。辛滨和辛酸有限的胞质氧化应激响应于H 2 O 2 。只有辛滨能够突出由抗霉素A诱导的MTROS产生的氧化胁迫。 Mitotempo和Sinapine都改善了IR后的心功能恢复。这与心脏组织内的较低的ROS生产相关。结论SINAPININ,一种天然阳离子亲水性酚,通常和基本上在油菜籽种类中发现,有效地(i)进入线粒体内,(ii)选择性地降低线粒体氧化应激的水平,(iii)有效地限制了心脏缺血期间的ROS生产 - 再灌注。

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