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通过临床代谢组学鉴定出N(8)-乙酰亚精胺作为斯奈德-罗宾逊综合征的潜在血浆生物标志物。

N(8)-acetylspermidine as a potential plasma biomarker for Snyder-Robinson syndrome identified by clinical metabolomics.

作者信息

Abela Lucia, Simmons Luke, Steindl Katharina, Schmitt Bernhard, Mastrangelo Massimo, Joset Pascal, Papuc Mihaela, Sticht Heinrich, Baumer Alessandra, Crowther Lisa M, Mathis Déborah, Rauch Anita, Plecko Barbara

机构信息

Division of Child Neurology, University Children's Hospital Zurich, Steinwiesstrasse 75, 8032, Zurich, Switzerland.

Children's Research Centre, University Children's Hospital Zurich, Steinwiesstrasse 75, 8032, Zurich, Switzerland.

出版信息

J Inherit Metab Dis. 2016 Jan;39(1):131-7. doi: 10.1007/s10545-015-9876-y. Epub 2015 Jul 15.

Abstract

Clinical metabolomics has emerged as a powerful tool to study human metabolism in health and disease. Comparative statistical analysis of untargeted metabolic profiles can reveal perturbations of metabolite levels in diseases and thus has the potential to identify novel biomarkers. Here we have applied a simultaneous genetic-metabolomic approach in twin boys with epileptic encephalopathy of unclear etiology. Clinical exome sequencing identified a novel missense mutation in the spermine synthase gene (SMS) that causes Snyder-Robinson syndrome (SRS). Untargeted plasma metabolome analysis revealed significantly elevated levels of N(8)-acetylspermidine, a precursor derivative of spermine biosynthesis, as a potential novel plasma biomarker for SRS. This result was verified in a third patient with genetically confirmed SRS. This study illustrates the potential of metabolomics as a translational technique to support exome data on a functional and clinical level.

摘要

临床代谢组学已成为研究健康和疾病状态下人类代谢的有力工具。对非靶向代谢谱进行比较统计分析,可以揭示疾病中代谢物水平的扰动,因此有潜力识别新的生物标志物。在此,我们对病因不明的癫痫性脑病双胞胎男孩应用了一种同时进行基因-代谢组学的方法。临床外显子组测序在精胺合酶基因(SMS)中发现了一个导致斯奈德-罗宾逊综合征(SRS)的新错义突变。非靶向血浆代谢组分析显示,精胺生物合成的前体衍生物N(8)-乙酰亚精胺水平显著升高,作为SRS潜在的新型血浆生物标志物。这一结果在第三例基因确诊的SRS患者中得到了验证。本研究说明了代谢组学作为一种转化技术在功能和临床层面支持外显子组数据的潜力。

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