首页> 外文期刊>Drug delivery and translational research >A facile approach for fabricating CD44-targeted delivery of hyaluronic acid-functionalized PCL nanoparticles in urethane-induced lung cancer: Bcl-2, MMP-9, caspase-9, and BAX as potential markers
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A facile approach for fabricating CD44-targeted delivery of hyaluronic acid-functionalized PCL nanoparticles in urethane-induced lung cancer: Bcl-2, MMP-9, caspase-9, and BAX as potential markers

机译:用于在氨基甲酸酯诱导的肺癌中制造透明质酸官能化PCL纳米颗粒的CD44靶向递送的容易方法:Bcl-2,MMP-9,Caspase-9和Bax作为潜在标记

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Lung carcinoma ranks highest in cancer-related death (about 20% of total cancer deaths) due to poor prognosis and lack of efficient management therapy. Owing to the lack of effective therapeutic approaches, survival rate of less than 5years persists over the years among non-small cell lung cancer (NSCLC) patients. Capsaicin (CAP) is well reported for its antiproliferative and antioxidant properties in various literature but lacks an appropriate delivery carrier. The present study was aimed to develop CAP-loaded hyaluronic acid (HA) nanoparticles (NPs) utilizing layer by layer technique to achieve enhanced and precise delivery as well as target specificity. The NPs were evaluated for in vitro release, particle size, zeta potential, and cytotoxicity on A549 cells. The optimized NPs exhibited a particle size of 1942.90nm, -27.873.21mV zeta potential, and 80.70 +/- 4.29% release, respectively, over a period of 48h. Flow cytometric analysis revealed superior performance of HA-PCL-CAP in terms of suppressed cell viability in A549 cell lines when compared with CAP and PCL-CAP. Further, HA-anchored NPs were evaluated in vivo for their therapeutic efficacy in urethane-induced lung carcinoma in rat model. The superlative therapeutic potential of HA-PCL-CAP was advocated from the results of reactive oxygen species and mitochondrial membrane-mediated apoptosis. HA-PCL-CAP-administered groups presented greater therapeutic efficacy as revealed through reduced tumor volume and improved animal survival rate. A greater drug accumulation in tumor tissue as revealed from biodistribution studies evidences targeting potential of HA-PCL-CAP in urethane-induced lung carcinoma.
机译:由于预后差和缺乏有效的管理治疗,肺癌在癌症相关死亡中排名最高(癌症总死亡的20%)。由于缺乏有效的治疗方法,多年来非小细胞肺癌(NSCLC)患者多年来,生存率少于5年。辣椒素(帽)良好地报道其各种文献中的抗增殖和抗氧化特性,但缺乏适当的递送载体。本研究旨在通过层技术开发帽加载的透明质酸(HA)纳米颗粒(NPS),以实现增强和精确的递送以及靶特异性。在A549细胞上评估NPS的体外释放,粒度,ζ电位和细胞毒性。优化的NPS在48h的时间内分别显示出1942.90nm,-27.873.21mVζ电位和80.70 +/- 4.29%的粒度。流式细胞术分析显示与帽和PCL帽相比,在A549细胞系中的抑制细胞活力方面揭示了HA-PCL-帽的优异性能。此外,在大鼠模型中的氨基甲酸酯诱导肺癌中的治疗疗效评估HA锚定NPS。 HA-PCL-帽的高级治疗潜力从反应性氧物质和线粒体膜介导的凋亡的结果提倡。 Ha-PCL-Cop-施用的基团呈现出更大的治疗效果,如通过降低的肿瘤体积和改善的动物存活率揭示。生物分布研究中揭示的肿瘤组织中的更大药物积累证据证明了氨基甲烷诱导的肺癌中HA-PCL-帽的靶向潜力。

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