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首页> 外文期刊>Biotechnology and Bioengineering >Delivery of Apoptotic Signal to Rolling Cancer Cells: A Novel Biomimetic Technique Using Immobilized TRAIL and E-Selectin
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Delivery of Apoptotic Signal to Rolling Cancer Cells: A Novel Biomimetic Technique Using Immobilized TRAIL and E-Selectin

机译:凋亡信号传递到滚动的癌细胞:一种新型的仿生技术,使用固定的TRAIL和E-选择素

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The survival rate for patients with metastases -versus localized cancer is dramatically reduced, with most deaths being associated with the formation of secondary tumors. Circulating cancer cells interact with the endothelial lining of the vasculature via a series of adhesive interactions that facilitate tethering and firm adhesion of cancer cells in the initial steps of metastasis. TNF-related apoptosisinducing ligand (TRAIL) holds promise as a tumor-specific cancer therapeutic, by inducing a death signal by apoptosis via the caspase pathway. In this study, we exploit this phenomenon to deliver a receptor-mediated apoptosis signal to leukemic cells adhesively rolling along a TRAIL and selectin-bearing surface. Results show that cancer cells exhibit selectin-mediated rolling in capillary flow chambers, and that the rolling velocities can be controlled by varying the selectin and electin surface density and the applied shear stress. It was determined that a 1 h rolling exposure to a functionalized TRAIL and E-selectin surface was sufficient to kill 30% of captured cells compared to static conditions in which 4 h exposure was necessary to kill 30% of the cells. Thus, we conclude that rolling delivery is more effective than static exposure to a TRAIL immobilized surface. We have also verified that there is no significant effect of TRAIL on hematopoietic stem cells and other normal blood cells. This represents the first demonstration of a novel biomimetic method to capture metastatic cells from circulation and deliver an apoptotic signal.
机译:与局部转移的癌症相比,转移患者的生存率显着降低,大多数死亡与继发性肿瘤的形成有关。循环癌细胞通过一系列粘附相互作用与脉管系统的内皮层相互作用,这些相互作用在转移的初始步骤中促进癌细胞的束缚和牢固粘附。 TNF相关的凋亡诱导配体(TRAIL)通过经由胱天蛋白酶途径通过凋亡诱导死亡信号而有望作为肿瘤特异性癌症治疗剂。在这项研究中,我们利用这种现象将受体介导的凋亡信号传递给沿着TRAIL和选择素表面滚动的白血病细胞。结果表明,癌细胞在毛细管流动腔中表现出选择素介导的滚动,并且可以通过改变选择素和电子素的表面密度以及所施加的剪切应力来控制滚动速度。已确定,与需要4小时暴露以杀死30%细胞的静态条件相比,对功能化TRAIL和E-选择素表面滚动暴露1 h足以杀死30%的捕获细胞。因此,我们得出结论,滚动传送比静态暴露于TRAIL固定表面更有效。我们还证实,TRAIL对造血干细胞和其他正常血细胞没有显着影响。这代表了一种新型仿生方法的首次演示,该方法可从循环中捕获转移性细胞并传递凋亡信号。

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