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Anti-platelet agents augment cisplatin nanoparticle cytotoxicity by enhancing tumor vasculature permeability and drug delivery

机译:抗血小板药通过增强肿瘤血管通透性和药物传递来增强顺铂纳米颗粒的细胞毒性

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摘要

Tumor vasculature is critically dependent on platelet mediated hemostasis and disruption of the same can augment delivery of nano-formulation based chemotherapeutic agents which depend on enhanced permeability and retention for tumor penetration. Here, we evaluated the role of Clopidogrel, a well-known inhibitor of platelet aggregation, in potentiating the tumor cytotoxicity of cisplatin nano-formulation in a murine breast cancer model. In vivo studies in murine syngeneic 4T1 breast cancer model showed a significant greater penetration of macromolecular fluorescent nanoparticles after clopidogrel pretreatment. Compared to selfassembling cisplatin nanoparticles (SACNs), combination therapy with clopidogrel and SACN was associated with a 4 fold greater delivery of cisplatin to tumor tissue and a greater reduction in tumor growth as well as higher survival rate. Clopidogrel enhances therapeutic efficiency of novel cisplatin based nano-formulations agents by increasing tumor drug delivery and can be used as a potential targeting agent for novel nano-formulation based chemotherapeutics.
机译:肿瘤脉管系统严重依赖于血小板介导的止血,而其破坏可以增加基于纳米制剂的化学治疗剂的递送,所述化学制剂依赖于增加的渗透性和对于肿瘤渗透的保留。在这里,我们评估了氯吡格雷(一种众所周知的血小板聚集抑制剂)在增强小鼠乳腺癌模型中顺铂纳米制剂的肿瘤细胞毒性中的作用。在小鼠同系4T1乳腺癌模型中进行的体内研究表明,氯吡格雷预处理后,大分子荧光纳米粒子的穿透力显着提高。与自组装的顺铂纳米颗粒(SACNs)相比,氯吡格雷和SACN的联合治疗将顺铂向肿瘤组织的转运增加4倍,肿瘤生长的减少更大,存活率更高。氯吡格雷通过增加肿瘤药物的输送量来提高新型基于顺铂的纳米制剂的治疗效率,并可用作潜在的靶向剂,用于新型基于纳米制剂的化学治疗。

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