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用于高通量药物筛选和疾病建模的血管化隐窝模式化结肠模型。

A vascularized crypt-patterned colon model for high-throughput drug screening and disease modelling.

机构信息

School of Biomedical Engineering, McMaster University, 1280 Main Street West, Hamilton, ON, L8S 4L8, Canada.

Department of Chemical Engineering, McMaster University, 1280 Main Street West, Hamilton, ON, L8S 4L8, Canada.

出版信息

Lab Chip. 2023 Jul 25;23(15):3370-3387. doi: 10.1039/d3lc00211j.

DOI:10.1039/d3lc00211j
PMID:37335565
Abstract

The colon serves as a primary target for pharmaceutical compound screening and disease modelling. To better study colon diseases and develop treatments, engineered models with colon-specific physiological features are required. Existing colon models lack integration of colonic crypt structures with underlying perfusable vasculature, where vascular-epithelial crosstalk is affected by disease progression. We present a colon epithelium barrier model with vascularized crypts that recapitulates relevant cytokine gradients in both healthy and inflammatory conditions. Using our previously published IFlowPlate384 platform, we initially imprinted crypt topography and populated the patterned scaffold with colon cells. Proliferative colon cells spontaneously localized to the crypt niche and differentiated into epithelial barriers with a tight brush border. Toxicity of the colon cancer drug, capecitabine, was tested and showed a dose-dependent response and recovery from crypt-patterned colon epithelium exclusively. Perfusable microvasculature was then incorporated around the colon crypts followed by treatment with pro-inflammatory TNFα and IFNγ cytokines to simulate inflammatory bowel disease (IBD)-like conditions. We observed -like stromal basal-to-apical cytokine gradients in tissues with vascularized crypts and gradient reversals upon inflammation. Taken together, we demonstrated crypt topography integrated with underlying perfusable microvasculature has significant value for emulating colon physiology and in advanced disease modelling.

摘要

结肠是药物化合物筛选和疾病建模的主要靶标。为了更好地研究结肠疾病和开发治疗方法,需要具有结肠特异性生理特征的工程模型。现有的结肠模型缺乏与可灌注血管底层的结肠隐窝结构的整合,其中血管-上皮细胞的串扰受到疾病进展的影响。我们提出了一种具有血管化隐窝的结肠上皮屏障模型,该模型可重现健康和炎症条件下相关细胞因子的梯度。使用我们之前发表的 IFlowPlate384 平台,我们首先对隐窝的地形进行了压印,并在图案化支架上填充了结肠细胞。增殖性结肠细胞自发地定位于隐窝龛位,并分化为具有紧密刷状边界的上皮屏障。我们测试了结肠癌药物卡培他滨的毒性,结果显示其具有剂量依赖性反应,并且仅从隐窝图案化的结肠上皮中恢复。然后在结肠隐窝周围加入可灌注的微血管,并用促炎细胞因子 TNFα 和 IFNγ 处理,以模拟炎症性肠病(IBD)样条件。我们观察到血管化隐窝组织中存在基底至顶端的基质细胞因子梯度,并在炎症时出现梯度反转。总之,我们证明了与可灌注微血管整合的隐窝地形对于模拟结肠生理学和先进的疾病建模具有重要价值。

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