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Aminomalonic acid: identification in Escherichia coli and atherosclerotic plaque.

机译:氨基丙二酸:在大肠杆菌和动脉粥样硬化斑块中鉴定。

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摘要

Aminomalonic acid (Ama) has been isolated from proteins of Escherichia coli and human atherosclerotic plaque. The presence of Ama has important biological implications because the malonic acid moiety potentially imparts calcium binding properties to protein. Ama was obtained by anaerobic alkaline hydrolysis and identified by chromatographic behavior, quantitative acid-mediated decarboxylation to glycine, and unambiguous gas chromatographic/mass spectral detection. The chromatographic, chemical, and mass spectral properties of naturally occurring Ama were identical to those of the synthetic compound. Amino acid analysis and GC/mass spectrometry also revealed the presence of beta-carboxyaspartic acid and gamma-carboxyglutamic acid in the base hydrolysate of human atherosclerotic plaque. The ratio of Ama to beta-carboxyaspartic acid to gamma-carboxyglutamic acid was 20:1:10, and the quantity of Ama per 1,000 glycine residues was 0.2. Ama is a relatively unstable, minor amino acid in complex structures such as bacteria or tissues. This may explain why it has escaped detection previously, despite intensive investigation.
机译:氨基丙二酸(Ama)已从大肠杆菌和人的动脉粥样硬化斑块蛋白中分离出来。 Ama的存在具有重要的生物学意义,因为丙二酸部分可能赋予蛋白质钙结合特性。 Ama通过厌氧碱性水解获得,并通过色谱行为,定量的酸介导的脱羧成甘氨酸和明确的气相色谱/质谱检测来鉴定。天然存在的Ama的色谱,化学和质谱性质与合成化合物的相同。氨基酸分析和GC /质谱分析还揭示了人动脉粥样斑块的碱性水解产物中存在β-羧基天冬氨酸和γ-羧基谷氨酸。 Ama与β-羧基天冬氨酸和γ-羧基谷氨酸的比例为20:1:10,每1000个甘氨酸残基的Ama数量为0.2。在复杂结构(例如细菌或组织)中,Ama是相对不稳定的次要氨基酸。这可能解释了尽管进行了深入调查,但为何以前无法进行检测。

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