Advancement of Sialyltransferase Inhibitors: Therapeutic Challenges and Opportunities

被引:55
|
作者
Szabo, Remi [1 ]
Skropeta, Danielle [1 ,2 ]
机构
[1] Univ Wollongong, Sch Chem, Wollongong, NSW 2522, Australia
[2] Univ Wollongong, Ctr Med & Mol Biosci, Wollongong, NSW 2522, Australia
关键词
sialyltransferase inhibitors; structure-based design; anticancer agents; antimetastasis; diagnostic tools; CMP-SIALIC ACID; N-ACETYLNEURAMINIC ACID; BETA-D-GALACTOSIDE; EXPERIMENTAL PULMONARY METASTASIS; TRANSITION-STATE ANALOGS; FREE CLICK CHEMISTRY; CELL-SURFACE; POLYSIALIC ACID; BREAST-CANCER; STRUCTURAL-ANALYSIS;
D O I
10.1002/med.21407
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Hypersialylation of tumor cell surface proteins along with a marked upregulation of sialyltransferase (ST) activity is a well-established hallmark of cancer. Due to the critical role of STs in tumor growth and progression, ST inhibition has emerged as a potential new antimetastatic strategy for a range of cancers including pancreatic and ovarian. Human STs are divided into subtypes based on their linkage and acceptor molecule, with each subtype controlling the synthesis of specific sialylated structures with unique biological roles. This has important implications for inhibitor development, as STs also play significant roles in immune responses, inflammation, viral infection, and neurological disorders. Thus, the current goal in order to advance to the clinic is the development of subtype selective, cell-permeable and synthetically accessible, small-molecule ST inhibitors. Herein is a comprehensive review of the latest developments in ST inhibitors from design, Nature, and high-throughput screening, addressing both the challenges and opportunities in targeting cell surface sialylation. The review features an overview of the biological evaluation methods, computational and imaging tools, inhibitor molecular diversity, and selectivity toward ST subtypes, along with the emerging role of ST inhibitors as diagnostic tools for disease imaging. (C) 2016 Wiley Periodicals, Inc.
引用
收藏
页码:219 / 270
页数:52
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