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High Payload Dual Therapeutic-Imaging Nanocarriers for Triggered Tumor Delivery

机译:高效载荷双治疗 - 成像纳米载体用于触发肿瘤递送

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摘要

The in vitro and in vivo characterization of an optimized formulation of nanoparticles (NPs) loaded with a high content of dexamethasone palmitate (DEX-P), a chemotherapeutic adjuvant that decreases interstitial fluid pressure in tumors, and 111In, a signaling agent, is described. These NPs are uniform in size and composition. Single photon emission computed tomography imaging demonstrates significant tumor uptake of 111In-labeled DEX-P NPs in tumor-bearing mice. As with many nanoparticle-based drug delivery systems, significant liver accumulation is observed. Assessment of liver histology and blood tests show no apparent hepatic or renal toxicity of the DEX-P NPs. Conversion of DEX-P to DEX occurs when DEX-P NPs are incubated with mouse plasma, human tumor homogenate and ascites from tumor bearing mice, but not with human plasma. This conversion is slower in plasma from Es1e(−/−)/SCID mice, a potential alternative animal model that better mimics humans; however, plasma from these mice are not completely devoid of esterase activity. The difference between blood and tumor esterase activity in humans facilitates the delivery of DEX-P NPs to tumors and the release of dexamethasone by an esterase trigger.
机译:纳米颗粒(NPs)的优化配方的体外和体内特性,该纳米颗粒负载了高含量的地塞米松棕榈酸酯(DEX-P),一种可降低肿瘤间质液压力的化学佐剂和 111 其中,描述了一种信号传导剂。这些NP的大小和组成是一致的。单光子发射计算机断层扫描显像显示荷瘤小鼠中大量摄取 111 In标记的DEX-P NP。与许多基于纳米颗粒的药物递送系统一样,观察到明显的肝脏蓄积。肝组织学和血液测试的评估表明,DEX-P NPs没有明显的肝或肾毒性。当将DEX-P NP与小鼠血浆,人肿瘤匀浆和来自荷瘤小鼠的腹水温育而不与人血浆一起温育时,DEX-P向DEX的转化就会发生。 Es1 e(-/-) / SCID小鼠的血浆中这种转化较慢,这是一种更好地模仿人类的潜在替代动物模型。然而,来自这些小鼠的血浆并非完全没有酯酶活性。人体血液和肿瘤酯酶活性之间的差异促进了DEX-P NP向肿瘤的递送以及地塞米松通过酯酶触发的释放。

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