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首页> 外文期刊>Glycobiology. >Regulatory role of glycans in the control of hypoxia-driven angiogenesis and sensitivity to anti-angiogenic treatment.
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Regulatory role of glycans in the control of hypoxia-driven angiogenesis and sensitivity to anti-angiogenic treatment.

机译:聚糖在控制缺氧引起的血管生成和对抗血管生成治疗的敏感性中的调节作用。

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摘要

Abnormal glycosylation is a typical hallmark of the transition from healthy to neoplastic tissues. Although the importance of glycans and glycan-binding proteins in cancer-related processes such as tumor cell adhesion, migration, metastasis and immune escape has been largely appreciated, our awareness of the impact of lectin-glycan recognition in tumor vascularization is relatively new. Regulated glycosylation can influence vascular biology by controlling trafficking, endocytosis and signaling of endothelial cell (EC) receptors including vascular endothelial growth factor receptors, platelet EC adhesion molecule, Notch and integrins. In addition, glycans may control angiogenesis by regulating migration of endothelial tip cells and influencing EC survival and vascular permeability. Recent evidence indicated that changes in the EC surface glycome may also serve "on-and-off" switches that control galectin binding to signaling receptors by displaying or masking-specific glycan epitopes. These glycosylation-dependent lectin-receptor interactions can link tumor hypoxia to EC signaling and control tumor sensitivity to anti-angiogenic treatment.
机译:糖基化异常是从健康组织向肿瘤组织过渡的典型标志。尽管聚糖和聚糖结合蛋白在癌症相关过程(例如肿瘤细胞粘附,迁移,转移和免疫逃逸)中的重要性已广为人知,但我们对凝集素-聚糖识别在肿瘤血管形成中的影响的认识相对较新。调节的糖基化可通过控制内皮细胞(EC)受体(包括血管内皮生长因子受体,血小板EC粘附分子,Notch和整联蛋白)的运输,内吞作用和信号传导来影响血管生物学。另外,聚糖可通过调节内皮尖端细胞的迁移并影响EC存活和血管通透性来控制血管生成。最近的证据表明,EC表面糖原的变化也可能通过显示或掩盖特定的聚糖表位来控制半乳糖凝集素与信号受体结合的“开关”开关。这些依赖糖基化的凝集素-受体相互作用可以将肿瘤缺氧与EC信号传导联系起来,并控制肿瘤对抗血管生成治疗的敏感性。

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