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大鼠体内L-组氨酸的降解。咪唑基丙酮酸、咪唑基乳酸和咪唑基丙酸的形成。

The degradation of L-histidine in the rat. The formation of imidazolylpyruvate, imidazolyl-lactate and imidazolylpropionate.

作者信息

Emes A V, Hassall H

出版信息

Biochem J. 1973 Nov;136(3):649-58. doi: 10.1042/bj1360649.

DOI:10.1042/bj1360649
PMID:4360716
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1166000/
Abstract
  1. Soluble and mitochondrial forms of histidine-pyruvate aminotransferase were separated from rat liver preparations by chromatography on DEAE-cellulose. 2. These enzymes were characterized with respect to substrate specificity, substrate affinity, pH optimum, stability and molecular weight by chromatography on Sephadex G-200. 3. Each enzyme has a relatively broad specificity showing significant activity towards l-phenylalanine and l-tyrosine and catalysing transamination with a number of monocarboxylic 2-oxo acids. 2-Oxoglutarate is not a substrate for either enzyme. 4. The molecular weights of the two enzymes, by chromatography on Sephadex G-200, are in the range 130000-150000. 5. The formation in vitro of imidazolyl-lactate from imidazolylpyruvate and NADH was demonstrated by using liver preparations. 6. From a study of imidazolyl-lactate-NAD(+) oxidoreductase activity after electrophoresis of liver preparations on polyacrylamide gel, and from an examination of the activity of l-lactate-NAD(+) oxidoreductase (EC 1.1.1.27) towards imidazolylpyruvate, it is concluded that this latter enzyme is responsible for the formation of imidazolyl-lactate in the liver. 7. Preparations of bacteria obtained from rat faeces form imidazolylpropionate from l-histidine and urocanate without further subculture. The amount of imidazolylpropionate formed is increased under anaerobic conditions and more so in an atmosphere of H(2). It is suggested that the gut flora of the rat contribute largely, if not exclusively, to the formation of imidazolylpropionate normally found in the urine.
摘要
  1. 通过在DEAE - 纤维素上进行色谱分离,从大鼠肝脏制剂中分离出了组氨酸 - 丙酮酸转氨酶的可溶性形式和线粒体形式。2. 通过在Sephadex G - 200上进行色谱分析,对这些酶的底物特异性、底物亲和力、最适pH、稳定性和分子量进行了表征。3. 每种酶都具有相对广泛的特异性,对L - 苯丙氨酸和L - 酪氨酸表现出显著活性,并催化与多种单羧酸2 - 氧代酸的转氨基作用。2 - 氧代戊二酸不是这两种酶的底物。4. 通过在Sephadex G - 200上进行色谱分析,这两种酶的分子量在130000 - 150000范围内。5. 利用肝脏制剂证明了在体外由咪唑基丙酮酸和NADH形成咪唑基乳酸。6. 通过对肝脏制剂在聚丙烯酰胺凝胶上进行电泳后咪唑基乳酸 - NAD(+)氧化还原酶活性的研究,以及对L - 乳酸 - NAD(+)氧化还原酶(EC 1.1.1.27)对咪唑基丙酮酸活性的检测,得出结论:后一种酶负责肝脏中咪唑基乳酸的形成。7. 从大鼠粪便中获得的细菌制剂在未进一步传代培养的情况下,由L - 组氨酸和尿刊酸形成咪唑基丙酸。在厌氧条件下形成的咪唑基丙酸量增加,在H(2)气氛中增加得更多。有人提出,大鼠的肠道菌群在很大程度上(如果不是唯一的话)促成了通常在尿液中发现的咪唑基丙酸的形成。

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