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Amino-Functionalized Silica Nanoparticles: In Vitro Evaluation for Targeted Delivery and Therapy of Pancreatic Cancer

机译:氨基功能化二氧化硅纳米粒子:靶向评估和胰腺癌的体外评价。

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摘要

We report a method of synthesis and optimization of amino-functionalized silica nanoparticles (SiNPs) and their in vitro evaluation as targeted delivery vehicles for the potential treatment of pancreatic cancer. SiNPs can efficiently encapsulate doxorubicin and can be attached to a targeting moiety such as anti-Claudin-4 (CLN4). The preferential uptake in pancreatic cancer cells, where CLN4 is overexpressed, of SiNPs when conjugated to CLN4 antibody (compared to nonconjugated SiNPs) was confirmed by confocal microscopy. SiNPs encapsulating doxorubicin had greater efficacy in MTT assays than free doxorubicin, and when conjugated to CLN4, the efficacy was dramatically increased (at 1 μM). No apparent carrier toxicity was observed when void SiNPs were used. SiNPs carrying a chemotherapeutic drug have the potential to be used as a targeted therapy for lethal cancers, such as pancreatic cancer. Also, incorporation of fluorescent probes in these SiNPs creates the possibility of their use as an imaging probe for diagnostic purposes.
机译:我们报告了一种合成和优化氨基官能化的二氧化硅纳米粒子(SiNPs)的方法,以及它们的体外评估作为潜在的胰腺癌治疗的靶向载体。 SiNP可以有效地封装阿霉素,并且可以连接到靶向部分,例如抗Claudin-4(CLN4)。通过共聚焦显微镜证实了与CLN4抗体结合后(比未结合的SiNPs多),胰腺癌细胞中优先吸收CLN4的SiNPs。包裹阿霉素的SiNP在MTT分析中比游离阿霉素具有更高的功效,并且与CLN4偶联后,功效显着提高(1μM)。当使用无效的SiNP时,没有观察到明显的载体毒性。携带化学治疗药物的SiNP有潜力用作致死性癌症(例如胰腺癌)的靶向治疗。同样,将荧光探针掺入这些SiNP中也有可能将其用作诊断目的的成像探针。

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    《Journal of nanotechnology》 |2013年第2013期|1.1-1.8|共8页
  • 作者单位

    Pharmaceutical Research Institute at Albany College of Pharmacy and Health Sciences, 1 Discovery Drive, Rensselaer, NY 12144, USA;

    Pharmaceutical Research Institute at Albany College of Pharmacy and Health Sciences, 1 Discovery Drive, Rensselaer, NY 12144, USA;

    Pharmaceutical Research Institute at Albany College of Pharmacy and Health Sciences, 1 Discovery Drive, Rensselaer, NY 12144, USA;

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