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异戊酸血症中异常的三羧酸循环代谢产物。

Abnormal tricarboxylic acid cycle metabolites in isovaleric acidaemia.

作者信息

Loots D T

机构信息

School for Physical and Chemical Sciences, Centre of Metabolomics, Division of Biochemistry, North-West University, Hoffman Street, Private Bag X6001, Box 269, Potchefstroom 2531, South Africa.

出版信息

J Inherit Metab Dis. 2009 Jun;32(3):403-11. doi: 10.1007/s10545-009-1071-6. Epub 2009 Apr 5.

Abstract

BACKGROUND

Although a number of abnormal diagnostic metabolites have previously been described in the urine of patients with isovaleric acidaemia (IVA), they do not fully explain the clinical symptoms associated with this disease.

METHODS

On the basis of our current understanding of the TCA cycle and IVA, we predicted a number of abnormal methylated TCA cycle metabolites, initiated by methylsuccinic acid. We subsequently obtained characteristic gas chromatography-mass spectrometry elution times and mass spectra of the chemically synthesized predicted compounds and screened the urine of 6 IVA patients and 24 age-matched controls. Further proof for our findings was generated from a series of in vitro enzyme reactions using the chemically synthesized standards as substrates to their respective TCA cycle enzymes.

RESULTS

Apart from the previously described methylsuccinic and methylfumaric acid, 3-methylmalic acid, (2R,3S)- and (2R,3R)-methylcitric acid and 2-methyl-cis-aconitic acid were detected in the urine of all 6 IVA patients in increased amounts. Additionally, although not directly determined, the in vitro enzyme reaction using of 3-methylmalic acid and malate dehydrogenase, in conjunction with the detection of 2-ketobutyric acid in the urine of all 6 IVA patients, strongly suggests an additional synthesis of 3-methyloxaloacetic acid by the same cycle.

CONCLUSION

Not only do these newly identified metabolites serve as additional diagnostic markers to those previously identified in IVA, but due to the structural arrangements of the (2R,3R)-methylcitric acid and 2-methyl-cis-aconitinic acid-derived 2-methylisocitric acid, inhibition of normal TCA cycle metabolism results at citrate synthase and isocitrate dehydrogenase, respectively.

SYNOPSIS

Methylsuccinic acid acts as the initiating substrate to a series of abnormal, potentially harmful, methylated tricarboxylic acid cycle metabolites in isovaleric acidaemia.

摘要

背景

尽管先前已在异戊酸血症(IVA)患者的尿液中描述了多种异常诊断性代谢物,但它们并不能完全解释与该疾病相关的临床症状。

方法

基于我们目前对三羧酸循环和IVA的理解,我们预测了一些由甲基琥珀酸引发的异常甲基化三羧酸循环代谢物。随后,我们获得了化学合成的预测化合物的特征性气相色谱 - 质谱洗脱时间和质谱,并对6例IVA患者和24例年龄匹配的对照者的尿液进行了筛查。我们使用化学合成标准品作为各自三羧酸循环酶的底物进行了一系列体外酶反应,为我们的发现提供了进一步的证据。

结果

除了先前描述的甲基琥珀酸和甲基富马酸外,在所有6例IVA患者的尿液中均检测到3 - 甲基苹果酸、(2R,3S) - 和(2R,3R) - 甲基柠檬酸以及2 - 甲基 - 顺乌头酸的含量增加。此外,尽管未直接测定,但使用3 - 甲基苹果酸和苹果酸脱氢酶的体外酶反应,以及在所有6例IVA患者尿液中检测到2 - 氧代丁酸,强烈表明同一循环中额外合成了3 - 甲基草酰乙酸。

结论

这些新鉴定的代谢物不仅可作为IVA中先前鉴定的代谢物之外的额外诊断标志物,而且由于(2R,3R) - 甲基柠檬酸和2 - 甲基 - 顺乌头酸衍生的2 - 甲基异柠檬酸的结构排列,分别导致柠檬酸合酶和异柠檬酸脱氢酶处正常三羧酸循环代谢受到抑制。

概要

在异戊酸血症中,甲基琥珀酸作为一系列异常的、潜在有害的甲基化三羧酸循环代谢物的起始底物。

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