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Nihon Masu Sukuriningu Gakkai shi = Journal of Japanese Society for Mass-Screening最新文献

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Newborn screening and diagnosis of mucopolysaccharidoses: application of tandem mass spectrometry. 新生儿粘多糖病的筛查和诊断:串联质谱的应用。
Shunji Tomatsu, Francyne Kubaski, Kazuki Sawamoto, Robert W Mason, Eriko Yasuda, Tsutomu Shimada, Adriana M Montaño, Seiji Yamaguchi, Yasuyuki Suzuki, Tadao Orii

Mucopolysaccharidoses (MPS) are a group of lysosomal storage disorders caused by the deficiency of lysosomal enzymes. The enzymes are required to break down glycosaminoglycans (GAGs) that help build bone, cartilage, tendons, corneas, skin and connective tissue. In patients with MPS, a missing enzyme leads to the accumulation of GAGs in the cells, blood, connective tissues, and multiple organs. The consequence is permanent, with progressive cellular damage affecting patients' appearance, physical abilities, organ and system function, and skeletal and mental development. The measurement of each specific GAG in a variety of specimens is required to establish the correlation between GAGs and physiological status of patients and/or prognosis and pathogenesis of the disease and to separate the patients with MPS from the healthy controls. We have developed a highly accurate, sensitive, and cost-effective liquid chromatography tandem mass spectrometry (LC-MS/MS) method for measurements of disaccharides derived from four specific GAGs [chondroitin sulfate (CS), dermatan sulfate (DS), heparan sulfate (HS), and keratan sulfate (KS)]. Disaccharides were produced by specific enzyme digestion of each GAG, and subsequently, quantified by negative ion mode of multiple reaction monitoring. Subclasses of GAGs with the same molecular weights can be separated by liquid chromatography. We have also developed another GAG assay by high-throughput mass spectrometry (HT-MS/MS). The HT-MS/MS consists of an integrated solid phase extraction robot that binds and de-salts samples from assay plates and directly injects them into a MS/MS detector, reducing sample processing time to within ten seconds. HT-MS/MS consequently yields much faster throughput than conventional LC-MS/MS-based methods; however, the HT-MS/MS system does not use a chromatographic step, and therefore, cannot separate GAGs that have the same molecular weights. Both techniques can be applied to the analysis of dried blood spots, blood, and urine specimens. In this review, we describe the assay methods for GAGs and the application to newborn screening and diagnosis of MPS.

粘多糖病(MPS)是一种由溶酶体酶缺乏引起的溶酶体贮积性疾病。这些酶是分解糖胺聚糖(GAGs)所必需的,而糖胺聚糖有助于骨骼、软骨、肌腱、角膜、皮肤和结缔组织的形成。在MPS患者中,一种缺失的酶会导致gag在细胞、血液、结缔组织和多个器官中积累。其后果是永久性的,进行性细胞损伤影响患者的外观、身体能力、器官和系统功能以及骨骼和智力发育。为了建立GAG与患者生理状态和/或疾病的预后和发病机制之间的相关性,并将MPS患者与健康对照区分开,需要在各种标本中测量每种特异性GAG。我们开发了一种高精度、灵敏度高、成本效益高的液相色谱串联质谱(LC-MS/MS)方法,用于测量四种特定GAGs[硫酸软骨素(CS)、硫酸皮聚糖(DS)、硫酸肝素(HS)和硫酸角蛋白(KS)]衍生的双糖。每个GAG通过特定的酶切产生双糖,随后通过多重反应监测的负离子模式进行定量。具有相同分子量的gag亚类可以用液相色谱法分离。我们还开发了另一种高通量质谱(HT-MS/MS) GAG检测。HT-MS/MS由一个集成的固相萃取机器人组成,该机器人将分析板上的样品结合并脱盐,并直接将其注入MS/MS检测器,将样品处理时间缩短到10秒以内。因此,HT-MS/MS比传统的LC-MS/MS方法产生更快的吞吐量;然而,HT-MS/MS系统不使用色谱步骤,因此不能分离具有相同分子量的gag。这两种技术都可以应用于干血斑、血液和尿液标本的分析。本文就GAGs的检测方法及其在新生儿MPS筛查和诊断中的应用作一综述。
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Nihon Masu Sukuriningu Gakkai shi = Journal of Japanese Society for Mass-Screening
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