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首页> 外文期刊>International journal of nano and biomaterials >Hyaluronic acid carrier-cell interactions: a tri-culture model of the tumour microenvironment to study siRNA delivery under flow conditions
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Hyaluronic acid carrier-cell interactions: a tri-culture model of the tumour microenvironment to study siRNA delivery under flow conditions

机译:透明质酸载体细胞相互作用:肿瘤微环境的三培养模型,以研究流动条件下的siRNA递送

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CD44 is often over expressed in solid tumours, rendering this protein a ‘hot'target in drug delivery. As CD44 is the main surface receptor of hyaluronic acid (HA), one of the most common therapeutic approaches consists of hijacking the cell's mechanism of HA endocytosis to deliver active principles. This approach, however, presents two caveats: the poor understanding of HA-cell interactions and the ubiquitous expression of CD44 in other cell types, e.g., stromal cells. To predict the interaction of HA-decorated nanocarriers with CD44-expressing cells in the multi-cellular and complex tumour microenvironment, we have established a tri-culture, non-contact in vitro model (PANC-1 tumoural cells, HDF stromal cells, THP-1 macrophages) and quantified the delivery and kinetics of nanoparticle internalisation (via flow cytometry), investigating the system in both static and dynamic culturing conditions. We report that HA-decorated nanocarriers are able to preferentially deliver siRNA to pancreatic cancer cells, interestingly even under flow/dynamic conditions.
机译:CD44通常以实心肿瘤表达,使该蛋白质为“药物递送”。作为CD44是透明质酸(HA)的主要表面受体,最常见的治疗方法之一包括劫持细胞的HA内吞作用以提供活跃原理。然而,这种方法呈现了两种警告:对Ha-Cell相互作用的理解差和CD44在其他细胞类型中的无处不在的表达,例如基质细胞。为了预测HA装饰纳米载流子与CD44表达细胞在多细胞和复杂的肿瘤微环境中的相互作用,我们已经建立了三种培养,非接触体外模型(Panc-1巨核细胞,HDF基质细胞,THP -1巨噬细胞)并量化纳米粒子内化(通过流式细胞术)的输送和动力学,研究了静态和动态培养条件的系统。我们报告说,HA装饰的纳米载体能够优先将siRNA递送至胰腺癌细胞,即使在流动/动态条件下也是如此。

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