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溶解的肝脏细胞外基质在体外维持原代大鼠肝细胞表型。

Solubilized liver extracellular matrix maintains primary rat hepatocyte phenotype in-vitro.

作者信息

Loneker Abigail E, Faulk Denver M, Hussey George S, D'Amore Antonio, Badylak Stephen F

机构信息

Department of Bioengineering, University of Pittsburgh, Pittsburgh, Pennsylvania.

McGowan Institute for Regenerative Medicine, University of Pittsburgh, Pittsburgh, Pennsylvania.

出版信息

J Biomed Mater Res A. 2016 Apr;104(4):957-65. doi: 10.1002/jbm.a.35636. Epub 2016 Jan 13.

Abstract

Whole organ engineering and cell-based regenerative medicine approaches are being investigated as potential therapeutic options for end-stage liver failure. However, a major challenge of these strategies is the loss of hepatic specific function after hepatocytes are removed from their native microenvironment. The objective of the present study was to determine if solubilized liver extracellular matrix (ECM), when used as a media supplement, can better maintain hepatocyte phenotype compared to type I collagen alone or solubilized ECM harvested from a non-liver tissue source. Liver extracellular matrix (LECM) from four different species was isolated via liver tissue decellularization, solubilized, and then used as a media supplement for primary rat hepatocytes (PRH). The four species of LECM investigated were human, porcine, canine and rat. Cell morphology, albumin secretion, and ammonia metabolism were used to assess maintenance of hepatocyte phenotype. Biochemical and mechanical characterization of each LECM were also conducted. Results showed that PRH's supplemented with canine and porcine LECM maintained their phenotype to a greater extent compared to all other groups. PRH's supplemented with canine and porcine LECM showed increased bile production, increased albumin production, and the formation of multinucleate cells. The findings of the present study suggest that solubilized liver ECM can support in-vitro hepatocyte culture and should be considered for therapeutic and diagnostic techniques that utilize hepatocytes.

摘要

全器官工程和基于细胞的再生医学方法正在作为终末期肝衰竭的潜在治疗选择进行研究。然而,这些策略的一个主要挑战是肝细胞从其天然微环境中移除后肝特异性功能的丧失。本研究的目的是确定与单独使用I型胶原或从非肝脏组织来源收获的可溶性细胞外基质(ECM)相比,作为培养基补充剂使用的可溶性肝脏细胞外基质是否能更好地维持肝细胞表型。通过肝脏组织去细胞化分离出四种不同物种的肝脏细胞外基质(LECM),使其溶解,然后用作原代大鼠肝细胞(PRH)的培养基补充剂。所研究的四种LECM分别是人、猪、犬和大鼠的。细胞形态、白蛋白分泌和氨代谢用于评估肝细胞表型的维持情况。还对每种LECM进行了生化和力学特性分析。结果表明,与所有其他组相比,添加犬和猪LECM的PRH在更大程度上维持了其表型。添加犬和猪LECM的PRH胆汁生成增加、白蛋白生成增加且形成了多核细胞。本研究结果表明,可溶性肝脏ECM可支持体外肝细胞培养,应考虑将其用于利用肝细胞的治疗和诊断技术。

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