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Cardiolipin fingerprinting of leukocytes by MALDI-TOF/MS as a screening tool for Barth syndrome

机译:MALDI-TOF / MS对白细胞的心磷脂指纹图谱作为Barth综合征的筛查工具

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摘要

Barth syndrome (BTHS), an X-linked disease associated with cardioskeletal myopathy, neutropenia, and organic aciduria, is characterized by abnormalities of cardiolipin (CL) species in mitochondria. Diagnosis of the disease is often compromised by lack of rapid and widely available diagnostic laboratory tests. The present study describes a new method for BTHS screening based on MALDI-TOF/MS analysis of leukocyte lipids. This generates a "CL fingerprint" and allows quick and simple assay of the relative levels of CL and monolysocardiolipin species in leukocyte total lipid profiles. To validate the method, we used vector algebra to analyze the difference in lipid composition between controls (24 healthy donors) and patients (8 boys affected by BTHS) in the high-mass phospholipid range. The method of lipid analysis described represents an important additional tool for the diagnosis of BTHS and potentially enables therapeutic monitoring of drug targets, which have been shown to ameliorate abnormal CL profiles in cells.
机译:Barth综合征(BTHS)是与心脏骨骼肌病,中性粒细胞减少和有机酸尿症相关的X连锁疾病,其特征在于线粒体中的心磷脂(CL)种类异常。缺乏快速且广泛可用的诊断实验室测试通常会损害疾病的诊断。本研究描述了一种基于MALDI-TOF / MS分析白细胞脂质的BTHS筛选新方法。这将产生“ CL指纹”,并允许快速,简单地分析白细胞总脂质谱中的CL和单糖基心磷脂种类的相对水平。为了验证该方法,我们使用矢量代数分析了高质量磷脂范围内对照组(24位健康供体)和患者(8位受BTHS影响的男孩)之间的脂质组成差异。所描述的脂质分析方法代表了诊断BTHS的重要附加工具,并潜在地实现了对药物靶标的治疗性监测,这些药物靶标已被证明可以改善细胞中异常的CL谱。

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