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皮下人肝组织的时变结构和功能特征描述。

Time-dependent structural and functional characterization of subcutaneous human liver tissue.

机构信息

Department of Surgery, Nagasaki University Graduate School of Biomedical Sciences, Nagasaki, Japan.

出版信息

J Tissue Eng Regen Med. 2018 Dec;12(12):2287-2298. doi: 10.1002/term.2761. Epub 2018 Nov 19.

DOI:10.1002/term.2761
PMID:30353697
Abstract

Subcutaneous transplantation of engineered hepatocyte/fibroblast sheets (EHFSs) is a low invasive and safe approach to construct vascularized subcutaneous human liver tissue (VSLT). However, the liver-specific structures and functionalities in the development process of VSLTs in mice remain poorly understood. Here, we describe time-dependent characteristics of the formation of the vascular network, cell-cell adhesions, liver transporters, liver-specific protein synthesis, and metabolizing activities. The EHFSs formed multilayered thick tissues by rapid neovascularization, which allows overcoming extremely difficult problems, such as the lack of oxygen supply on the formation of three-dimensional primary hepatocyte tissue under the skin. The blood vessels consisted of mouse-origin endothelial cells (ECs) (mVEGFR2) from the subcutaneous space at 1-7 days, and the following formation of the vascular network was performed by human-origin ECs (hVEGFR2). Many varieties of liver-specific gene expressions increased with the construction of the VSLTs: cell-cell adhesion molecules (CDH1, CLDN3, and CX32), transporters at basal (OATP1A1, OCT1, and NTCP) and apical membranes (MRP2, MDR1, and BSEP), blood coagulation factors (F8 and F9), urea synthesis (CPS1, OTC, and ARG1), and metabolism enzymes (CYP7A1, CYP1A2, CYP2B6, CYP3A4, and UGT1A1). Subacute hepatic failure model mice with VSLT were alive at least 7 weeks after liver damage. Thus, the ectopic liver organ offers the potential for a low invasive and safe treatment for liver diseases.

摘要

工程化肝细胞/成纤维细胞片(EHFS)的皮下移植是构建血管化皮下人肝组织(VSLT)的一种低侵入性和安全的方法。然而,在小鼠中 VSLT 发展过程中肝脏特异性结构和功能仍知之甚少。在这里,我们描述了血管网络形成、细胞-细胞黏附、肝脏转运体、肝脏特异性蛋白合成和代谢活性的时间依赖性特征。EHFS 通过快速新生血管化形成多层厚组织,这使得克服了极其困难的问题成为可能,例如在皮肤下形成三维原代肝细胞组织时缺乏氧气供应。血管由皮下空间中的鼠源性内皮细胞(mVEGFR2)组成(1-7 天),随后由人源性内皮细胞(hVEGFR2)形成血管网络。随着 VSLT 的构建,许多种类的肝脏特异性基因表达增加:细胞-细胞黏附分子(CDH1、CLDN3 和 CX32)、基底膜(OATP1A1、OCT1 和 NTCP)和顶膜(MRP2、MDR1 和 BSEP)转运体、凝血因子(F8 和 F9)、尿素合成(CPS1、OTC 和 ARG1)和代谢酶(CYP7A1、CYP1A2、CYP2B6、CYP3A4 和 UGT1A1)。具有 VSLT 的亚急性肝衰竭模型小鼠在肝损伤后至少存活 7 周。因此,异位肝器官为肝脏疾病的低侵入性和安全治疗提供了潜力。

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