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一种用于研究细菌癌症靶向的新型微流控共培养系统。

A novel microfluidic co-culture system for investigation of bacterial cancer targeting.

机构信息

Division of Mechanical Engineering, School of Mechanical, Aerospace and Systems Engineering, KAIST, 291 Daehak-ro, Yuseong-gu, Daejeon, Republic of Korea.

出版信息

Lab Chip. 2013 Aug 7;13(15):3033-40. doi: 10.1039/c3lc50163a.

DOI:10.1039/c3lc50163a
PMID:23743709
Abstract

Although bacterial cancer targeting in animal models has been previously demonstrated and suggested as a possible therapeutic tool, a thorough understanding of the mechanisms responsible for cancer specificity would be required prior to clinical applications. To visualize bacterial preference for cancer cells over normal cells and to elucidate the cancer-targeting mechanism, a simple microfluidic platform has been developed for in vitro studies. This platform allows simultaneous cultures of multiple cell types in independent culture environments in isolated chambers, and creates a stable chemical gradient across a collagen-filled passage between each of these cell culture chambers and the central channel. The established chemical gradient induces chemotactic preferential migration of bacteria toward a particular cell type for quantitative analysis. As a demonstration, we tested differential bacterial behavior on a two-chamber device where we quantified bacterial preference based on the difference in fluorescence intensities of green fluorescence protein (GFP)-expressing bacteria at two exits of the collagen-filled passages. Analysis of the chemotactic behavior of Salmonella typhimurium toward normal versus cancer hepatocytes using the developed platform revealed an apparent preference for cancer hepatocytes. We also demonstrate that alpha-fetoprotein (AFP) is one of the key chemo-attractants for S. typhimurium in targeting liver cancer.

摘要

虽然在动物模型中已经证明了细菌对癌症的靶向作用,并将其作为一种潜在的治疗工具进行了研究,但在临床应用之前,需要深入了解导致癌症特异性的机制。为了可视化细菌对癌细胞的偏好,阐明癌症靶向机制,我们开发了一种简单的微流控平台用于体外研究。该平台允许在独立的培养环境中同时培养多种细胞类型,并在这些细胞培养室和中央通道之间的填充有胶原蛋白的通道中形成稳定的化学梯度。建立的化学梯度诱导细菌向特定细胞类型进行趋化性优先迁移,以进行定量分析。作为一个演示,我们在一个两室设备上测试了细菌的差异行为,我们根据绿色荧光蛋白(GFP)表达细菌在胶原蛋白填充通道两个出口处的荧光强度差异来量化细菌的偏好。使用开发的平台分析鼠伤寒沙门氏菌对正常和肝癌细胞的趋化行为,发现其对肝癌细胞有明显的偏好。我们还证明,甲胎蛋白(AFP)是沙门氏菌靶向肝癌的关键趋化因子之一。

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