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Targeting C-type lectin receptors with multivalent carbohydrate ligands

机译:用多价碳水化合物配体靶向C型凝集素受体

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摘要

C-type lectin receptors (CLRs) represent a large receptor family including collectins, selectins, lymphocyte lectins, and proteoglycans. CLRs share a structurally homologous carbohydrate-recognition domain (CRD) and often bind carbohydrates in a Ca2+-dependent manner. In innate immunity, CLRs serve as pattern recognition receptors (PRRs) and bind to the glycan structures of pathogens and also to self-antigens. In nature, the low affinity of CLR/carbohydrate interactions is overcome by multivalent ligand presentation at the surface of cells or pathogens. Thus, multivalency is a promising strategy for targeting CLR-expressing cells and, indeed, carbohydrate-based targeting approaches have been employed for a number of CLRs, including asialoglycoprotein receptor (ASGPR) in the liver, or DC-SIGN expressed by dendritic cells. Since CLR engagement not only mediates endocytosis but also influences intracellular signaling pathways, CLR targeting may allow for cell-specific drug delivery and also the modulation of cellular functions. Glyconanoparticles, glycodendrimers, and glycoliposomes were successfully used as tools for CLR-specific targeting. This review will discuss different approaches for multivalent CLR ligand presentation and aims to highlight how CLR targeting has been employed for cell specific drug delivery. Major emphasis is directed towards targeting of CLRs expressed by antigen-presenting cells to modulate immune responses.
机译:C型凝集素受体(CLR)代表一个大的受体家族,包括collectin,selectins,淋巴细胞凝集素和蛋白聚糖。 CLR共享结构上同源的碳水化合物识别域(CRD),并且通常以Ca2 +依赖的方式结合碳水化合物。在先天免疫中,CLR充当模式识别受体(PRR),并与病原体的聚糖结构以及自身抗原结合。在自然界中,CLR /碳水化合物相互作用的低亲和力可通过在细胞或病原体表面上呈现多价配体来克服。因此,多价是靶向表达CLR的细胞的有前途的策略,并且事实上,基于碳水化合物的靶向方法已经用于许多CLR,包括肝脏中的去唾液酸糖蛋白受体(ASGPR)或树突状细胞表达的DC-SIGN。由于CLR参与不仅介导内吞作用,而且还影响细胞内信号传导途径,因此CLR靶向可能允许细胞特异性药物递送以及细胞功能调节。糖基纳米颗粒,糖类树状聚合物和糖脂质体已成功用作CLR特异性靶向的工具。这篇综述将讨论用于多价CLR配体呈递的不同方法,并旨在强调如何将CLR靶向用于细胞特异性药物递送。主要重点在于靶向抗原呈递细胞表达的CLR以调节免疫应答。

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