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首页> 外文期刊>Molecular genetics and metabolism >Heparan sulfate and dermatan sulfate derived disaccharides are sensitive markers for newborn screening for mucopolysaccharidoses types I, II and III
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Heparan sulfate and dermatan sulfate derived disaccharides are sensitive markers for newborn screening for mucopolysaccharidoses types I, II and III

机译:硫酸乙酰肝素和硫酸皮肤素衍生的二糖是新生儿筛查I,II和III型粘多糖酶的敏感标志物

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Introduction: Mucopolysaccharidoses (MPSs) are a group of lysosomal storage disorders (LSDs) caused by a defect in the degradation of glycosaminoglycans (GAGs). The accumulation of GAGs in MPS patients results in extensive, severe and progressive disease. Disease modifying therapy is available for three of the MPSs and is being developed for the other types. Early initiation of treatment, before the onset of irreversible tissue damage, clearly provides a favorable disease outcome. However, early diagnosis is difficult due to the rarity of these disorders in combination with the wide variety of clinical symptoms. Newborn screening (NBS) is probably the optimal approach, and several screening techniques for different MPSs have been studied. Here we describe a relatively simple and sensitive method to measure levels of dermatan and heparan sulfate derived disaccharides in dried blood spots (DBS) with HPLC-MS/MS, and show that this reliably separates MPS I, II and MPS III newborns from controls and heterozygotes. Methods: Newborn DBS of 11 MPS I, 1 MPS II, and 6 MPS III patients, with phenotypes ranging from severe to relatively attenuated, were collected and levels of dermatan and heparan sulfate derived disaccharides in these DBS were compared with levels in DBS of newborn MPS I and MPS III heterozygotes and controls. Results: The levels of dermatan and heparan sulfate derived disaccharides were clearly elevated in all newborn DBS of MPS I, II and III patients when compared to controls. In contrast, DBS of MPS I and III heterozygotes showed similar disaccharide levels when compared to control DBS. Conclusions: Our study demonstrates that measurement of heparan and dermatan sulfate derived disaccharides in DBS may be suitable for NBS for MPS I, II and MPS III. We hypothesize that this same approach will also detect MPS VI, and VII patients, as heparan sulfate and/or dermatan sulfate is also the primary storage products in these disorders.
机译:简介:粘多糖贮积酶(MPS)是由糖胺聚糖(GAG)降解缺陷引起的一组溶酶体贮积病(LSD)。 MPS患者中GAG的积累导致广泛,严重和进行性疾病。疾病改良疗法可用于三种MPS,并且正在针对其他类型进行开发。在发生不可逆的组织损伤之前,尽早开始治疗显然可以提供有利的疾病预后。但是,由于这些疾病的罕见性以及多种临床症状的结合,很难进行早期诊断。新生儿筛查(NBS)可能是最佳方法,并且已经研究了几种针对不同MPS的筛查技术。在这里,我们描述了一种相对简单而灵敏的方法,用HPLC-MS / MS测量干血斑(DBS)中皮肤素和硫酸乙酰肝素衍生的二糖的水平,并表明该方法可靠地将MPS I,II和MPS III新生儿与对照组和杂合子。方法:收集11名MPS I,1名MPS II和6名MPS III型患者的新生儿DBS,表型从严重到相对减弱,并比较这些DBS中皮肤素和硫酸乙酰肝素衍生的二糖的水平与新生儿DBS的水平MPS I和MPS III杂合子和对照。结果:与对照组相比,MPS I,II和III患者的所有新生儿DBS中皮肤素和硫酸乙酰肝素衍生的二糖水平均明显升高。相反,与对照DBS相比,MPS I和III杂合子的DBS显示出相似的二糖水平。结论:我们的研究表明,DBS中乙酰肝素和硫酸皮肤素二糖的测定可能适用于MPS I,II和MPS III的NBS。我们假设这种相同的方法也可以检测MPS VI和VII患者,因为硫酸乙酰肝素和/或硫酸皮肤素也是这些疾病的主要储存产物。

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