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Syndecans in chronic inflammatory and autoimmune diseases: Pathological insights and therapeutic opportunities

机译:慢性炎症和自身免疫性疾病中的Syndecans:病理学见解和治疗机会

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摘要

Syndecans (SDCs) are a family of heparan sulfate proteoglycans (HSPGs) glycoproteins ubiquitously expressed on the cell surfaces and extracellular matrix of all mammalian tissues. There are four mammalian syndecans, SDC-1 thorough 4, which play a critical role in cell adhesion, migration, proliferation, differentiation, and angiogenesis through independent and growth factor mediated signaling. An altered expression of SDCs is often observed in autoimmune disorders, cancer, HIV infection, and many other pathological conditions. SDCs modulate disease progression by interacting with a diverse array of ligands, receptors, and other proteins, including extracellular matrix, glycoproteins, integrins, morphogens, and various growth factors and chemokines, along with their receptors and kinases. Specifically, SDCs present on cell surface can bind directly to chemokines to enhance their binding to receptors, downstream signaling, and migration. Alternatively, SDCs can be cleaved and shed to mediate negative regulation of chemokine and growth factor signaling pathways and ligand sequestration. Importantly, SDC shedding may be a biomarker of inflammation, especially in chronic inflammatory diseases. While the current therapies for cancer and several autoimmune disorders have revolutionized treatment outcomes, understanding the pathophysiological role of SDCs and the use of HSPG mimetic or antagonists on cytokine signaling networks may uncover potentially novel targeted therapeutic approaches. This review mainly summarizes the current findings on the role of individual SDCs in disease processes, mechanisms through which SDCs mediate their biological functions, and the possibility of targeting SDCs as future potential therapeutic approaches.
机译:Syndecans(SDC)是在所有哺乳动物组织的细胞表面和细胞外基质上普遍表达的硫酸乙酰肝素蛋白聚糖(HSPG)糖蛋白家族。 SDC-1共有4种哺乳动物共癸,它们通过独立的生长因子介导的信号传导在细胞粘附,迁移,增殖,分化和血管生成中发挥关键作用。通常在自身免疫性疾病,癌症,HIV感染和许多其他病理状况中观察到SDC表达的改变。 SDC通过与各种配体,受体和其他蛋白质(包括细胞外基质,糖蛋白,整联蛋白,吗啡原,各种生长因子和趋化因子)以及它们的受体和激酶相互作用而调节疾病进程。具体而言,存在于细胞表面的SDC可以直接结合趋化因子,从而增强其与受体的结合,下游信号传导和迁移。或者,可以切割和脱落SDC以介导趋化因子和生长因子信号传导途径以及配体螯合的负调节。重要的是,SDC脱落可能是炎症的生物标志,尤其是在慢性炎症性疾病中。尽管目前的癌症治疗方法和几种自身免疫性疾病已经彻底改变了治疗结果,但了解SDC的病理生理作用以及在细胞因子信号网络上使用HSPG模拟物或拮抗剂可能会发现潜在的新型靶向治疗方法。这篇综述主要总结了有关单个SDC在疾病过程中的作用,SDC介导其生物学功能的机制以及将SDC作为未来潜在治疗方法的可能性的当前发现。

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