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非环氧化酶衍生前列腺素的定量分析作为氧化应激的标志物

Quantification of noncyclooxygenase derived prostanoids as a marker of oxidative stress.

作者信息

Morrow J D, Roberts L J

机构信息

Department of Pharmacology, Vanderbilt University, Nashville, TN 37232-6602.

出版信息

Free Radic Biol Med. 1991;10(3-4):195-200. doi: 10.1016/0891-5849(91)90076-f.

Abstract

Recently, we discovered there is a unique class of prostaglandin F2-like compounds that are formed in vitro from arachidonoyl-containing lipids in plasma by a free radical-catalyzed mechanism. More recent studies have elucidated that these prostanoids are also produced in vivo in humans by a similar noncyclooxygenase mechanism. Levels of these PGF2 compounds detected by a mass spectrometric assay in normal human plasma and urine range from approximately 5-50 pg/mL and 500-3000 pg/mg creatinine, respectively. Circulating levels of the compounds were shown to increase by as much as 200-fold in animal models of free radical-induced lipid peroxidation. These results suggest that quantification of these prostanoids may provide a new approach to assess oxidative stress in vivo in humans. Potential advantages of this approach are that the mass spectrometric assay has a high degree of sensitivity, accuracy, and specificity and the assay can be used to quantitate these compounds in a variety of biological fluids. In addition, quantification of these compounds is of interest because these compounds possess biological activity. Disadvantages of the assay are the potential of ex vivo formation of these compounds in biological fluids containing lipids and, further, these compounds must be differentiated from PGF2 compounds that are formed via the cyclooxygenase enzyme. In addition, because the levels of these compounds in normal human plasma and urine are relatively high, assaying these compounds in circulating plasma and urine may be somewhat insensitive for the detection of increased production at isolated sites of oxidant injury within the body, in which case sampling near localized sites of their formation may be required.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

最近,我们发现了一类独特的前列腺素F2样化合物,它们在体外由血浆中含花生四烯酰的脂质通过自由基催化机制形成。最近的研究表明,这些前列腺素类物质在人体内也通过类似的非环氧化酶机制在体内产生。通过质谱分析在正常人血浆和尿液中检测到的这些PGF2化合物水平分别约为5 - 50 pg/mL和500 - 3000 pg/mg肌酐。在自由基诱导的脂质过氧化动物模型中,这些化合物的循环水平显示增加多达200倍。这些结果表明,对这些前列腺素类物质进行定量分析可能为评估人体内的氧化应激提供一种新方法。这种方法的潜在优势在于质谱分析具有高度的灵敏度、准确性和特异性,并且该分析可用于定量多种生物流体中的这些化合物。此外,对这些化合物进行定量分析很有意义,因为这些化合物具有生物活性。该分析的缺点是在含有脂质的生物流体中这些化合物有体外形成的可能性,而且,这些化合物必须与通过环氧化酶形成的PGF2化合物区分开来。此外,由于这些化合物在正常人血浆和尿液中的水平相对较高,在循环血浆和尿液中检测这些化合物对于检测体内孤立的氧化损伤部位产量增加可能有点不敏感,在这种情况下可能需要在其形成的局部部位附近取样。(摘要截断于250字)

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