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生物打印的3D原代人肠道组织模型体现了天然生理学和药物代谢动力学/药物毒性(ADME/Tox)功能的各个方面。

Bioprinted 3D Primary Human Intestinal Tissues Model Aspects of Native Physiology and ADME/Tox Functions.

作者信息

Madden Lauran R, Nguyen Theresa V, Garcia-Mojica Salvador, Shah Vishal, Le Alex V, Peier Andrea, Visconti Richard, Parker Eric M, Presnell Sharon C, Nguyen Deborah G, Retting Kelsey N

机构信息

Organovo, Inc., San Diego, CA 92121, USA.

Department of Pharmacokinetics, Merck & Co., Inc., Rahway, NJ 07065, USA.

出版信息

iScience. 2018 Apr 27;2:156-167. doi: 10.1016/j.isci.2018.03.015. Epub 2018 Mar 27.

Abstract

The human intestinal mucosa is a critical site for absorption, distribution, metabolism, and excretion (ADME)/Tox studies in drug development and is difficult to recapitulate in vitro. Using bioprinting, we generated three-dimensional (3D) intestinal tissue composed of human primary intestinal epithelial cells and myofibroblasts with architecture and function to model the native intestine. The 3D intestinal tissue demonstrates a polarized epithelium with tight junctions and specialized epithelial cell types and expresses functional and inducible CYP450 enzymes. The 3D intestinal tissues develop physiological barrier function, distinguish between high- and low-permeability compounds, and have functional P-gp and BCRP transporters. Biochemical and histological characterization demonstrate that 3D intestinal tissues can generate an injury response to compound-induced toxicity and inflammation. This model is compatible with existing preclinical assays and may be implemented as an additional bridge to clinical trials by enhancing safety and efficacy prediction in drug development.

摘要

在药物研发中,人体肠道黏膜是吸收、分布、代谢和排泄(ADME)/毒性研究的关键部位,且难以在体外进行重现。利用生物打印技术,我们构建了由人原代肠上皮细胞和成肌纤维细胞组成的三维(3D)肠道组织,其结构和功能可模拟天然肠道。该3D肠道组织呈现出具有紧密连接和特殊上皮细胞类型的极化上皮,并表达功能性和可诱导的CYP450酶。3D肠道组织具有生理屏障功能,能区分高渗透性和低渗透性化合物,且具有功能性P-糖蛋白和乳腺癌耐药蛋白转运体。生化和组织学特征表明,3D肠道组织可对化合物诱导的毒性和炎症产生损伤反应。该模型与现有的临床前检测方法兼容,通过提高药物研发中的安全性和疗效预测,可作为通向临床试验的额外桥梁。

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