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首页> 外文期刊>Angewandte Chemie >Antiadhesive Nanosomes Facilitate Targeting of the Lysosomal GlcNAc Salvage Pathway through Derailed Cancer Endocytosis
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Antiadhesive Nanosomes Facilitate Targeting of the Lysosomal GlcNAc Salvage Pathway through Derailed Cancer Endocytosis

机译:抗炎纳米体促进溶酶体glcnac救赎途径通过脱轨癌症内吞作用

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摘要

Activated endocytosis of extracellular macromolecules and their intracellular trafficking to lysosomes is an essential metabolic mechanism in cancer cells during their rapid proliferation. Cancer cells reuse a vast amount of N-acetylglucosamine (GlcNAc) supplied from the GlcNAc salvage pathway for the accelerated synthesis of a pivotal uridine diphosphate (UDP)-GlcNAc. A method to inactivate key glycosidases in lysosomes could critically contribute to the development of potent anticancer therapy. Here we demonstrate that "nanosomes" made of core metals covered by an antiadhesive mixed self-assembled monolayer allow for avoiding nonspecific surface protein corona and targeted molecular delivery through activated endocytosis. Nanosomes carrying suicide substrates showed that lysosomal glycosidases such as beta-hexosaminidase and beta-galactosidase in cancer cells are promising targets for novel anticancer therapeutic nanomedicine that induce apoptotic cell death through lysosomal membrane permeabilization. The advantage of this method is evident because multivalent surface loading by antiadhesive nanosomes makes it possible to highlight "weak interactions" such as carbohydrate-lectin interactions independent of surface protein corona.
机译:细胞外大分子的活性内吞作用及其细胞内贩运对溶酶体是癌细胞在快速增殖期间的基本代谢机制。癌细胞再利用从GlcNAc救赎途径提供的大量N-乙酰葡糖胺(GlcNAc),以加速合成枢轴尿苷二磷酸(UDP)-GLCNAc。在溶酶体中灭活关键糖苷酶的方法可能会对强化抗癌治疗的发展有贡献。在这里,我们证明了由抗炎混合混合的单层覆盖的芯金属制成的“纳米瘤”允许通过活化的内吞作用避免非特异性表面蛋白质电晕和靶向分子递送。承载自杀基材的纳米粒子表明,癌细胞中β-六氨基氨基氨基酶和β-半乳糖苷酶如β-六莨菪碱和β-半乳糖苷酶是有前途的,用于通过溶酶体膜透化诱导凋亡细胞死亡的新型抗癌治疗纳米疫苗。这种方法的优点是显而易见的,因为通过抗炎纳米体的多价表面负载使得可以突出诸如碳水化合物凝集素相互作用的“弱相互作用”,与表面蛋白质蛋白质无关。

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