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Genomic and functional characterization of stellate cells isolated from human cirrhotic livers.从人类肝硬化肝脏中分离出的星状细胞的基因组和功能特征
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Lipocalin 2 diminishes invasiveness and metastasis of Ras-transformed cells.脂质运载蛋白2可降低Ras转化细胞的侵袭性和转移性。
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肝纤维化进展过程中肝细胞类型特异性标记基因的基因表达谱

Gene expression profiles of hepatic cell-type specific marker genes in progression of liver fibrosis.

作者信息

Takahara Yoshiyuki, Takahashi Mitsuo, Wagatsuma Hiroki, Yokoya Fumihiko, Zhang Qing-Wei, Yamaguchi Mutsuyo, Aburatani Hiroyuki, Kawada Norifumi

机构信息

Exploratory and Applied Pharmaceutical Research Department, Pharmaceutical Company, Ajinomoto Co., Inc., 1-1 Suzuki-cho, Kawasaki-ku, Kawasaki 210-8681, Japan.

出版信息

World J Gastroenterol. 2006 Oct 28;12(40):6473-99. doi: 10.3748/wjg.v12.i40.6473.

DOI:10.3748/wjg.v12.i40.6473
PMID:17072980
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4100637/
Abstract

AIM

To determine the gene expression profile data for the whole liver during development of dimethylni-trosamine (DMN)-induced hepatic fibrosis.

METHODS

Marker genes were identified for different types of hepatic cells, including hepatic stellate cells (HSCs), Kupffer cells (including other inflammatory cells), and hepatocytes, using independent temporal DNA microarray data obtained from isolated hepatic cells.

RESULTS

The cell-type analysis of gene expression gave several key results and led to formation of three hypotheses: (1) changes in the expression of HSC-specific marker genes during fibrosis were similar to gene expression data in in vitro cultured HSCs, suggesting a major role of the self-activating characteristics of HSCs in formation of fibrosis; (2) expression of mast cell-specific marker genes reached a peak during liver fibrosis, suggesting a possible role of mast cells in formation of fibrosis; and (3) abnormal expression of hepatocyte-specific marker genes was found across several metabolic pathways during fibrosis, including sulfur-containing amino acid metabolism, fatty acid metabolism, and drug metabolism, suggesting a mechanistic relationship between these abnormalities and symptoms of liver fibrosis.

CONCLUSION

Analysis of marker genes for specific hepatic cell types can identify the key aspects of fibrogenesis. Sequential activation of inflammatory cells and the self-supporting properties of HSCs play an important role in development of fibrosis.

摘要

目的

确定二甲基亚硝胺(DMN)诱导的肝纤维化发展过程中全肝的基因表达谱数据。

方法

利用从分离的肝细胞获得的独立时间DNA微阵列数据,鉴定不同类型肝细胞的标记基因,包括肝星状细胞(HSCs)、库普弗细胞(包括其他炎症细胞)和肝细胞。

结果

基因表达的细胞类型分析得出了几个关键结果,并形成了三个假设:(1)纤维化过程中肝星状细胞特异性标记基因表达的变化与体外培养的肝星状细胞中的基因表达数据相似,表明肝星状细胞的自我激活特性在纤维化形成中起主要作用;(2)肥大细胞特异性标记基因的表达在肝纤维化期间达到峰值,表明肥大细胞在纤维化形成中可能起作用;(3)在纤维化过程中,在包括含硫氨基酸代谢、脂肪酸代谢和药物代谢在内的几个代谢途径中发现了肝细胞特异性标记基因的异常表达,表明这些异常与肝纤维化症状之间存在机制上的关系。

结论

对特定肝细胞类型的标记基因进行分析可以确定纤维化形成的关键方面。炎症细胞的顺序激活和肝星状细胞的自我支持特性在纤维化发展中起重要作用。