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首页> 外文期刊>Oxidative Medicine and Cellular Longevity >MitoCLox: A Novel Mitochondria-Targeted Fluorescent Probe for Tracing Lipid Peroxidation
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MitoCLox: A Novel Mitochondria-Targeted Fluorescent Probe for Tracing Lipid Peroxidation

机译:Mitoclox:一种用于追踪脂质过氧化的新型线粒体靶向荧光探针

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摘要

Peroxidation of cardiolipin (CL) in the inner mitochondrial membrane plays a key role in the development of various pathologies and, probably, aging. The four fatty acid tails of CL are usually polyunsaturated, which makes CL particularly sensitive to peroxidation. Peroxidation of CL is involved in the initiation of apoptosis, as well as in some other important cellular signaling chains. However, the studies of CL peroxidation are strongly limited by the lack of methods for its tracing in living cells. We have synthesized a new mitochondria-targeted fluorescent probe sensitive to lipid peroxidation (dubbed MitoCLox), where the BODIPY fluorophore, carrying a diene-containing moiety (as in the C11-BODIPY (581/591) probe), is conjugated with a triphenylphosphonium cation (TPP+) via a long flexible linker that contains two amide bonds. The oxidation of MitoCLox could be measured either as a decrease of absorbance at 588?nm or as an increase of fluorescence in the ratiometric mode at 520/590?nm (emission). In CL-containing liposomes, MitoCLox oxidation was induced by cytochrome c and developed in parallel with cardiolipin oxidation. TPP+-based mitochondria-targeted antioxidant SkQ1, in its reduced form, inhibited oxidation of MitoCLox concurrently with the peroxidation of cardiolipin. Molecular dynamic simulations of MitoCLox in a cardiolipin-containing membrane showed affinity of positively charged MitoCLox to negatively charged CL molecules; the oxidizable diene moiety of MitoCLox resided on the same depth as the cardiolipin lipid peroxides. We suggest that MitoCLox could be used for monitoring CL oxidation in vivo and, owing to its flexible linker, also serve as a platform for producing peroxidation sensors with affinity to particular lipids.
机译:内部线粒体膜中心肌素(Cl)的过氧化在各种病变的发展中起着关键作用,并且可能是老化。 Cl的四个脂肪酸尾通常是多不饱和的,这使得Cl对过氧化特别敏感。 Cl的过氧化参与凋亡的开始,以及一些其他重要的细胞信号链。然而,CL过氧化的研究受到在活细胞中缺乏其追踪的方法的强烈限制。我们已经合成了对脂质过氧化(被称为Mitoclox)敏感的新的线粒体靶向荧光探针,其中携带二烯部分的Bodipy荧光团(如在C11-Bodipy(581/591)探针中)与三苯基鏻缀合通过长柔性接头阳离子(TPP +),含有两个酰胺键。 Mitoclox的氧化可以测量为588Ω·Nm的吸光度降低,或者在520/590Ω(发射)下的比例模式中的荧光的增加。在含Cl的脂质体中,通过细胞色素C诱导Mitoclox氧化,并与心肝脂氧平行发展。 TPP +基于线粒体靶向抗氧化剂SKQ1,其形式还抑制了与心肝素的过氧化同时均匀的Mitoclox氧化。在含心脂蛋白的膜中Mitoclox的分子动态模拟显示出带正电荷的mitoclox与带负电的Cl分子的亲和力; Mitoclox的可氧化二烯部分仍居中与心脂素脂质过氧化物相同的深度。我们表明,Mitoclox可用于监测体内Cl氧化,并且由于其柔性接头,也用作生产对特定脂质的亲和力的过氧化传感器的平台。

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