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首页> 外文期刊>Macromolecular bioscience >Poly(ornithine-co-arginine-co-glycine-co-aspartic Acid): Preparation via NCA Polymerization and its Potential as a Polymeric Tumor-Penetrating Agent
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Poly(ornithine-co-arginine-co-glycine-co-aspartic Acid): Preparation via NCA Polymerization and its Potential as a Polymeric Tumor-Penetrating Agent

机译:聚(鸟氨酸-精氨酸-甘氨酸-天冬氨酸):通过NCA聚合制备及其作为肿瘤穿透剂的潜力

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摘要

A novel random copolypeptide of ornithine, arginine, glycine, and aspartic acid [Poly(ornithine-co-arginine-co-glycine-co-aspartic acid), Poly(O,R,G,D)] has been prepared through ring-opening polymerization of N--carbobenzoxy-l-ornithine N-carboxyanhydride [Orn(Cbz)-NCA)], l-glycine N-carboxyanhydride (Gly-NCA) and -benzyl l-aspartate N-carboxyanhydride [Asp(Bn)-NCA], following by subsequent deprotection and guanidization. The structure of Poly(O,R,G,D) was confirmed by nuclear magnetic resonance (NMR) spectroscopy and gel permeation chromatography (GPC). Low cytotoxicity of Poly(O,R,G,D) was confirmed from MTT assay. The Poly(O,R,G,D) contain some internal sequences of RXXR (X=O, R, G, or D) that could be proteolytically cleaved to expose the cryptic CendR element and bind to Neuropilin-1. This would lead to vascular and tissue permeabilization. Therefore trypsin-cleaved Poly(O,R,G,D) increase the vascular leakage of Evans blue from dermal microvessels at the injection site in vivo skin permeability assay. The intratumoral injection of the Poly(O,R,G,D) significantly enhanced the concentration of cisplatin-loaded nanoparticles in MCF-7 solid tumors. These results show that Poly(O,R,G,D) could increase the vascular leakage and tissue penetration of nanoparticles in a solid tumor and can be used as a potential polymeric tumor-penetrating agent.
机译:新型的鸟氨酸,精氨酸,甘氨酸和天冬氨酸[Poly(ornithine-co-精氨酸-co-glycine-co-天冬氨酸),Poly(O,R,G,D)]的随机无规多肽已经通过环N-碳苯甲氧基-1-鸟氨酸N-羧基酐[Orn(Cbz)-NCA],1-甘氨酸N-羧基酐(Gly-NCA)和-苄基1-天冬氨酸N-羧基酐[Asp(Bn)- NCA],随后进行脱保护和胍基化。聚(O,R,G,D)的结构通过核磁共振(NMR)光谱和凝胶渗透色谱(GPC)得以确认。通过MTT分析证实了聚(O,R,G,D)的低细胞毒性。 Poly(O,R,G,D)包含RXXR的一些内部序列(X = O,R,G或D),可以通过蛋白水解方式切割以暴露隐秘的CendR元件并与Neuropilin-1结合。这将导致血管和组织通透。因此,在体内皮肤渗透性测定中,胰蛋白酶切割的Poly(O,R,G,D)增加了注射部位伊文思蓝从真皮微血管的血管渗漏。瘤内注射Poly(O,R,G,D)可以显着提高MCF-7实体瘤中顺铂加载的纳米颗粒的浓度。这些结果表明,Poly(O,R,G,D)可以增加实体瘤中纳米颗粒的血管渗漏和组织渗透,并且可以用作潜在的聚合物肿瘤穿透剂。

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