Heparan-6-O-endosulfatase 2, a cancer-related proteoglycan enzyme, is effectively inhibited by a specific sea cucumber fucosylated glycosaminoglycan.

IF 3.4 3区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

Glycobiology Pub Date : 2025-04-23 DOI:10.1093/glycob/cwaf025

Marwa Farrag, Reem Aljuhani, Julius Benicky, Hoda Al Ahmed, Sandeep K Misra, Sushil K Mishra, Joshua S Sharp, Robert J Doerksen, Radoslav Goldman, Vitor H Pomin

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引用次数: 0

Abstract

Heparan-6-O-endosulfatase 2 (Sulf-2) is a proteoglycan enzyme that modifies sulfation of heparan sulfate proteoglycans. Dysregulation of Sulf-2 is associated with various pathological conditions, including cancer, which makes Sulf-2 a potential therapeutic target. Despite the key pathophysiological roles of Sulf-2, inhibitors remain insufficiently developed. In previous work, a fucosylated chondroitin sulfate from the sea cucumber Holothuria floridana (HfFucCS) exhibited potent Sulf-2 inhibition. This study investigates the structural basis of HfFucCS-mediated Sulf-2 inhibition, examines the binding profile of HfFucCS to Sulf-2, and explores the mode of inhibition. Additionally, a structurally diverse library of sulfated poly/oligosaccharides, including common glycosaminoglycans and unique marine sulfated glycans, was screened for Sulf-2 inhibition. Results from a high-throughput arylsulfatase assay and specific 6-O-desulfation assay have proved that HfFucCS is the most potent among the tested sulfated glycans, likely due to the presence of the unique 3,4-disulfated fucose structural motif. HfFucCS demonstrated non-competitive inhibition, and inhibitory analysis of its low-molecular-weight fragments suggests a minimum length of ~7.5 kDa for effective inhibition. Surface plasmon resonance analyses revealed that Sulf-2 binds to surface heparin with high affinity (KD of 0.817 nM). HfFucCS and its derivatives effectively disrupt this interaction. Results from mass spectrometry-hydroxyl radical protein footprinting and repulsive scaling replica exchange molecular dynamics indicate similarities in the binding of heparin and HfFucCS oligosaccharides to both the catalytic and hydrophilic domains of Sulf-2. These findings reveal the unique inhibitory properties of a structurally distinct marine glycosaminoglycan, supporting its further investigation as a selective and effective inhibitor for Sulf-2-associated cancer events.

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Heparan-6-O-endosulfatase 2是一种与癌症相关的蛋白聚糖酶，可被一种特定的海参聚焦糖胺聚糖有效抑制。

肝素-6- o -巯基内酯酶2（硫-2）是一种蛋白聚糖酶，可修饰硫酸肝素蛋白聚糖的磺化。硫-2的失调与包括癌症在内的各种病理状况有关，这使得硫-2成为潜在的治疗靶点。尽管硫-2具有关键的病理生理作用，但抑制剂的开发仍然不足。在先前的研究中，从佛罗里达海参（Holothuria florida, HfFucCS）中提取的一种浓缩硫酸软骨素表现出有效的硫-2抑制作用。本研究探讨了HfFucCS介导的硫-2抑制的结构基础，研究了HfFucCS与硫-2的结合谱，并探索了抑制模式。此外，我们还筛选了一个结构多样的磺化聚/寡糖文库，包括常见的糖胺聚糖和独特的海洋磺化聚糖，以抑制硫-2。高通量芳基磺化酶实验和特异性6- o -脱硫实验的结果证明，HfFucCS是所测试的磺化聚糖中最有效的，可能是由于存在独特的3,4-二硫化聚焦结构基序。HfFucCS表现出非竞争性抑制作用，对其低分子量片段的抑制分析表明，有效抑制的最小长度为~7.5 kDa。表面等离子体共振分析表明，硫-2与表面肝素具有高亲和力（KD为0.817 nM）。HfFucCS及其衍生物有效地破坏了这种相互作用。质谱-羟基自由基蛋白足迹和排斥尺度复制交换分子动力学的结果表明，肝素和HfFucCS低聚糖与硫-2的催化和亲水性结构域的结合具有相似性。这些发现揭示了一种结构独特的海洋糖胺聚糖的独特抑制特性，支持其作为硫-2相关癌症事件的选择性和有效抑制剂的进一步研究。

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来源期刊

Glycobiology 生物-生化与分子生物学

CiteScore

7.50

自引率

4.70%

发文量

审稿时长

3 months

期刊介绍： Established as the leading journal in the field, Glycobiology provides a unique forum dedicated to research into the biological functions of glycans, including glycoproteins, glycolipids, proteoglycans and free oligosaccharides, and on proteins that specifically interact with glycans (including lectins, glycosyltransferases, and glycosidases). Glycobiology is essential reading for researchers in biomedicine, basic science, and the biotechnology industries. By providing a single forum, the journal aims to improve communication between glycobiologists working in different disciplines and to increase the overall visibility of the field.