大鼠肝脏细胞外基质的分子成分对肝祖细胞组织修复的响应。

Peter Siig Vestentoft, Peter Jelnes, Jesper B Andersen, Thi Anh Thu Tran, Tenna Jørgensen, Morten Rasmussen, Jette Bornholdt, Lene Melsæther Grøvdal, Charlotte Harken Jensen, Lotte Katrine Vogel, Snorri S Thorgeirsson, Hanne Cathrine Bisgaard
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引用次数: 17

摘要

背景:成年哺乳动物肝脏的组织修复发生在两个不同的过程中,被称为第一级和第二级防御。当肝祖细胞(HPCs)对肝损伤作出第二层防御反应时,我们开始表征细胞外基质分子成分的变化。结果:我们对大鼠肝脏进行了转录谱分析,通过第一层(手术切除70%的肝块(PHx方案))和第二层(70%肝切除术结合暴露于2-乙酰氨基芴(AAF/PHx方案))对肝损伤进行了防御,并将未经治疗的大鼠肝脏(对照)与两种方案中肝切除术后第1天、第5天和第9天的肝脏的转录特征进行了比较。许多编码胶原蛋白、层粘连蛋白、整合素和各种其他细胞外基质结构成分的特定亚基的转录本被不同地上调或下调(P结论:转录谱分析和免疫检测,包括三维重建,产生了在肝损伤第二层防御中表达的细胞外基质成分的详细概述。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Molecular constituents of the extracellular matrix in rat liver mounting a hepatic progenitor cell response for tissue repair.

Background: Tissue repair in the adult mammalian liver occurs in two distinct processes, referred to as the first and second tiers of defense. We undertook to characterize the changes in molecular constituents of the extracellular matrix when hepatic progenitor cells (HPCs) respond in a second tier of defense to liver injury.

Results: We used transcriptional profiling on rat livers responding by a first tier (surgical removal of 70% of the liver mass (PHx protocol)) and a second tier (70% hepatectomy combined with exposure to 2-acetylaminofluorene (AAF/PHx protocol)) of defense to liver injury and compared the transcriptional signatures in untreated rat liver (control) with those from livers of day 1, day 5 and day 9 post hepatectomy in both protocols. Numerous transcripts encoding specific subunits of collagens, laminins, integrins, and various other extracellular matrix structural components were differentially up- or down-modulated (P < 0.01). The levels of a number of transcripts were significantly up-modulated, mainly in the second tier of defense (Agrn, Bgn, Fbn1, Col4a1, Col8a1, Col9a3, Lama5, Lamb1, Lamb2, Itga4, Igtb2, Itgb4, Itgb6, Nid2), and their signal intensities showed a strong or very strong correlation with Krt1-19, a well-established marker of a ductular/HPC reaction. Furthermore, a significant up-modulation and very strong correlation between the transcriptional profiles of Krt1-19 and St14 encoding matriptase, a component of a novel protease system, was found in the second tier of defense. Real-time PCR confirmed the modulation of St14 transcript levels and strong correlation to Krt-19 and also showed a significant up-modulation and strong correlation to Spint1 encoding HAI-1, a cognate inhibitor of matriptase. Immunodetection and three-dimensional reconstructions showed that laminin, Collagen1a1, agrin and nidogen1 surrounded bile ducts, proliferating cholangiocytes, and HPCs in ductular reactions regardless of the nature of defense. Similarly, matriptase and HAI-1 were expressed in cholangiocytes regardless of the tier of defense, but in the second tier of defense, a subpopulation of HPCs in ductular reactions co-expressed HAI-1 and the fetal hepatocyte marker Dlk1.

Conclusion: Transcriptional profiling and immunodetection, including three-dimensional reconstruction, generated a detailed overview of the extracellular matrix constituents expressed in a second tier of defense to liver injury.

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