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环加成反应:通往“双糖基化”的便捷途径

Cycloadditions as a Sweet Route to 'Double -Glycosylation'.

作者信息

Mahoney Kevin P P, Lynch Rosemary, Bown Rhea T, Sharma Sunil V, Chueakwon Piyasiri, Stephenson G Richard, Cordes David B, Slawin Alexandra M Z, Goss Rebecca J M

机构信息

School of Chemistry, Integrated Institute of Engineering, and BSRC, University of St. Andrews, St. Andrews KY16 9ST, UK.

TopChem Pharmaceuticals, Ballymote Business Park, Carrownanty, F56 RX08 Ballymote, Ireland.

出版信息

Biomolecules. 2025 Jun 19;15(6):905. doi: 10.3390/biom15060905.

Abstract

Pharmaceuticals, such as the antibiotic erythromycin, and sodium-dependent glucose transporter (SGLT1 & SGTL2) inhibitors such as Bexagliflozin (diabetes) and Sotagliflozin (heart disease), are often sugar-decorated (glycosylated). Glycosylation is a key component of the binding motif in SGLT inhibitors and, in natural products, glycosylation often confers improved bioactivity and bioavailability. Whilst a single -glycoside link between a sugar moiety and its aglycone core is a common feature in natural products isolated to date, only a small number, including the antibiotics granaticin and sarubicin, are covalently bonded twice to a single sugar moiety. The way in which this "double -glycosylation" is naturally mediated is not yet known, yet has been speculated on. Here, we report the exploration and development of a potentially biomimetic procedure that utilises intermolecular cycloaddition chemistry to access new "double -glycosylated" products and enables the creation of bridged polycyclic ethers from a common maltol-derived oxidopyrylium salt precursor.

摘要

药物,如抗生素红霉素,以及钠依赖性葡萄糖转运蛋白(SGLT1和SGLT2)抑制剂,如贝西格列净(用于治疗糖尿病)和索格列净(用于治疗心脏病),通常都进行了糖修饰(糖基化)。糖基化是SGLT抑制剂结合基序的关键组成部分,在天然产物中,糖基化通常会提高生物活性和生物利用度。虽然糖部分与其苷元核心之间的单糖苷键是迄今为止分离出的天然产物中的常见特征,但只有少数,包括抗生素格拉纳汀和沙鲁比星,与单个糖部分共价键合两次。这种“双糖基化”的自然介导方式尚不清楚,但已有推测。在此,我们报告了一种潜在的仿生方法的探索和开发,该方法利用分子间环加成化学来获得新的“双糖基化”产物,并能够从常见的麦芽酚衍生的氧化吡啶盐前体生成桥连多环醚。

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