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Detection of Active Mammalian GH31 α-Glucosidases in Health and Disease Using In-Class, Broad-Spectrum Activity-Based Probes

机译:使用类内,广谱活性探针检测健康和疾病中的活性哺乳动物GH31α-葡萄糖苷酶

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摘要

The development of small molecule activity-based probes (ABPs) is an evolving and powerful area of chemistry. There is a major need for synthetically accessible and specific ABPs to advance our understanding of enzymes in health and disease. α-Glucosidases are involved in diverse physiological processes including carbohydrate assimilation in the gastrointestinal tract, glycoprotein processing in the endoplasmic reticulum (ER), and intralysosomal glycogen catabolism. Inherited deficiency of the lysosomal acid α-glucosidase (GAA) causes the lysosomal glycogen storage disorder, Pompe disease. Here, we design a synthetic route for fluorescent and biotin-modified ABPs for in vitro and in situ monitoring of α-glucosidases. We show, through mass spectrometry, gel electrophoresis, and X-ray crystallography, that α-glucopyranose configured cyclophellitol aziridines label distinct retaining α-glucosidases including GAA and ER α-glucosidase II, and that this labeling can be tuned by pH. We illustrate a direct diagnostic application in Pompe disease patient cells, and discuss how the probes may be further exploited for diverse applications.
机译:基于小分子活性的探针(ABP)的开发是化学领域一个不断发展的强大领域。迫切需要合成可及的特定ABP,以增进我们对健康和疾病中酶的了解。 α-葡萄糖苷酶参与多种生理过程,包括胃肠道中的碳水化合物吸收,内质网(ER)中的糖蛋白加工以及溶酶体糖原分解代谢。溶酶体酸α-葡糖苷酶(GAA)的​​遗传缺陷会导致溶酶体糖原储存障碍,庞贝病。在这里,我们设计了一种荧光和生物素修饰的ABP的合成路线,用于体外和原位监测α-葡萄糖苷酶。我们通过质谱,凝胶电泳和X射线晶体学显示,α-吡喃葡萄糖配置的环磷脂醇氮丙啶标记了截然不同的保留α-葡萄糖苷酶,包括GAA和ERα-葡萄糖苷酶II,并且该标记可以通过pH来调节。我们说明了在庞贝病患者细胞中的直接诊断应用,并讨论了如何将探针进一步用于各种应用。

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