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一种用于评估淋巴管脂质转运的肠道乳糜管组织工程模型。

A tissue-engineered model of the intestinal lacteal for evaluating lipid transport by lymphatics.

作者信息

Dixon J Brandon, Raghunathan Sandeep, Swartz Melody A

机构信息

Institute of Bioengineering, School of Life Sciences, Ecole Polytechnique Fédérale de Lausanne, CH-1015 Lausanne, Switzerland.

出版信息

Biotechnol Bioeng. 2009 Aug 15;103(6):1224-35. doi: 10.1002/bit.22337.

Abstract

Lacteals are the entry point of all dietary lipids into the circulation, yet little is known about the active regulation of lipid uptake by these lymphatic vessels, and there lacks in vitro models to study the lacteal-enterocyte interface. We describe an in vitro model of the human intestinal microenvironment containing differentiated Caco-2 cells and lymphatic endothelial cells (LECs). We characterize the model for fatty acid, lipoprotein, albumin, and dextran transport, and compare to qualitative uptake of fatty acids into lacteals in vivo. We demonstrate relevant morphological features of both cell types and strongly polarized transport of fatty acid in the intestinal-to-lymphatic direction. We found much higher transport rates of lipid than of dextran or albumin across the lymphatic endothelial monolayer, suggesting most lipid transport is active and intracellular. This was confirmed with confocal imaging of Bodipy, a fluorescent fatty acid, along with transmission electron microscopy. Since our model recapitulates crucial aspects of the in vivo lymphatic-enterocyte interface, it is useful for studying the biology of lipid transport by lymphatics and as a tool for screening drugs and nanoparticles that target intestinal lymphatics.

摘要

乳糜管是所有膳食脂质进入循环系统的入口,但对于这些淋巴管对脂质摄取的主动调节知之甚少,并且缺乏研究乳糜管 - 肠上皮细胞界面的体外模型。我们描述了一种包含分化的Caco - 2细胞和淋巴管内皮细胞(LEC)的人肠道微环境体外模型。我们对该模型进行了脂肪酸、脂蛋白、白蛋白和右旋糖酐转运的表征,并与体内脂肪酸向乳糜管的定性摄取进行了比较。我们展示了两种细胞类型的相关形态特征以及脂肪酸在肠到淋巴方向上的强极化转运。我们发现脂质穿过淋巴管内皮单层的转运速率比右旋糖酐或白蛋白高得多,这表明大多数脂质转运是主动的且是细胞内的。这通过荧光脂肪酸Bodipy的共聚焦成像以及透射电子显微镜得到了证实。由于我们的模型概括了体内淋巴管 - 肠上皮细胞界面的关键方面,它对于研究淋巴管脂质转运生物学以及作为筛选靶向肠道淋巴管的药物和纳米颗粒的工具很有用。

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