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氨基酸、肽和蛋白质侧链及主链位点上形成的氢过氧化物的分离、检测和定量。

Separation, detection, and quantification of hydroperoxides formed at side-chain and backbone sites on amino acids, peptides, and proteins.

作者信息

Morgan Philip E, Pattison David I, Hawkins Clare L, Davies Michael J

机构信息

Free Radical Group, The Heart Research Institute, Camperdown, Sydney, NSW 2050, Australia.

出版信息

Free Radic Biol Med. 2008 Nov 1;45(9):1279-89. doi: 10.1016/j.freeradbiomed.2008.08.004. Epub 2008 Aug 8.

Abstract

Hydroperoxides are major reaction products of radicals and singlet oxygen with amino acids, peptides, and proteins. However, there are few data on the distribution of hydroperoxides in biological samples and their sites of formation on peptides and proteins. In this study we show that normal-or reversed-phase gradient HPLC can be employed to separate hydroperoxides present in complex systems, with detection by postcolumn oxidation of ferrous xylenol orange to the ferric species and optical detection at 560 nm. The limit of detection (10-25 pmol) is comparable to chemiluminescence detection. This method has been used to separate and detect hydroperoxides, generated by hydroxyl radicals and singlet oxygen, on amino acids, peptides, proteins, plasma, and intact and lysed cells. In conjunction with EPR spin trapping and LC/MS/MS, we have obtained data on the sites of hydroperoxide formation. A unique fingerprint of hydroperoxides formed at alpha-carbon (backbone) positions has been identified; such backbone hydroperoxides are formed in significant yields only when the amino acid is part of a peptide or protein. Only side-chain hydroperoxides are detected with free amino acids. These data indicate that free amino acids are poor models of protein damage induced by radicals or other oxidants.

摘要

氢过氧化物是自由基和单线态氧与氨基酸、肽和蛋白质反应的主要产物。然而,关于生物样品中氢过氧化物的分布及其在肽和蛋白质上的形成位点的数据却很少。在本研究中,我们表明,正相或反相梯度高效液相色谱法可用于分离复杂体系中存在的氢过氧化物,通过将亚铁二甲苯酚橙柱后氧化为铁离子并在560 nm处进行光学检测来实现。检测限(10 - 25 pmol)与化学发光检测相当。该方法已用于分离和检测由羟基自由基和单线态氧在氨基酸、肽、蛋白质、血浆以及完整和裂解细胞上产生的氢过氧化物。结合电子顺磁共振自旋捕集和液相色谱/串联质谱,我们获得了氢过氧化物形成位点的数据。已鉴定出在α-碳(主链)位置形成的氢过氧化物的独特指纹图谱;仅当氨基酸是肽或蛋白质的一部分时,此类主链氢过氧化物才会大量生成。游离氨基酸仅检测到侧链氢过氧化物。这些数据表明,游离氨基酸并不是自由基或其他氧化剂诱导蛋白质损伤的良好模型。

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