Quantitative characterization of specific targeting of tumor cells by antibody-functionalized particles

M. T. Stamm, Andrew S. Trickey-Glassman, Linan Jiang, Y. Zohar
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引用次数: 2

Abstract

Receptor-ligand binding has been one of the more popular approaches to specifically targeting tumor cells. In this work, targeting efficiency was quantitatively characterized using silica particles functionalized with EpCAM antibodies and EpCAM-expressing BT-20 breast cancer cells. The effects of incubation time and particle concentration on the number of functionalized particles bound to target cells were experimentally investigated. The number of bound particles was found to increase with particle concentration, but not necessarily with incubation time. While particle desorption and cellular loss of binding affinity in time seem to be negligible, cell-particle-cell interaction was identified as the limiting mechanism for the number of particles bound to target cells. The current findings suggest that separation of a bound particle from a cell may be detrimental to cellular binding affinity.
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抗体功能化颗粒特异性靶向肿瘤细胞的定量表征
受体-配体结合是目前比较流行的靶向肿瘤细胞的方法之一。在这项工作中,利用EpCAM抗体功能化的二氧化硅颗粒和表达EpCAM的BT-20乳腺癌细胞,定量表征了靶向效率。实验研究了孵育时间和颗粒浓度对结合靶细胞的功能化颗粒数量的影响。结合颗粒的数量随颗粒浓度的增加而增加,但与孵育时间无关。虽然颗粒解吸和细胞在时间上的结合亲和力损失似乎可以忽略不计,但细胞-颗粒-细胞相互作用被认为是结合靶细胞的颗粒数量的限制机制。目前的研究结果表明,结合颗粒从细胞中分离可能对细胞结合亲和力有害。
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