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来自基因改造动物的肝细胞生长因子- Met信号通路的生物学作用

Biological roles of hepatocyte growth factor-Met signaling from genetically modified animals.

作者信息

Kato Takashi

机构信息

Urologic Oncology Branch, National Cancer Institute, National Institute of Health, Bethesda, MD 20892, USA.

出版信息

Biomed Rep. 2017 Dec;7(6):495-503. doi: 10.3892/br.2017.1001. Epub 2017 Oct 18.

Abstract

Hepatocyte growth factor (HGF) is produced by stromal and mesenchymal cells, and it stimulates epithelial cell proliferation, motility, morphogenesis and angiogenesis in various organs via tyrosine phosphorylation of its cognate receptor, Met. The HGF-Met signaling pathway contributes in a paracrine manner to the development of epithelial organs, exerts regenerative effects on the epithelium, and promotes the regression of fibrosis in numerous organs. Additionally, the HGF-Met signaling pathway is correlated with the biology of cancer types, neurons and immunity. analyses using genetic modification have markedly increased the profound understanding of the HGF-Met system in basic biology and its clinical applications. HGF and Met knockout (KO) mice are embryonically lethal. Therefore, amino acids in multifunctional docking sites of Met have been exchanged with specific binding motifs for downstream adaptor molecules in order to investigate the signaling potential of the HGF-Met signaling pathway. Conditional Met KO mice were generated using Cre-loxP methodology and characterization of these mice indicated that the HGF-Met signaling pathway is essential in regeneration, protection, and homeostasis in various tissue types and cells. Furthermore, the results of studies using HGF-overexpressing mice have indicated the therapeutic potential of HGF for various types of disease and injury. In the present review, the phenotypes of gene-modified mice are summarized.

摘要

肝细胞生长因子(HGF)由基质细胞和间充质细胞产生,它通过其同源受体Met的酪氨酸磷酸化,刺激各种器官中的上皮细胞增殖、迁移、形态发生和血管生成。HGF-Met信号通路以旁分泌方式促进上皮器官的发育,对上皮发挥再生作用,并促进许多器官中纤维化的消退。此外,HGF-Met信号通路与癌症类型、神经元和免疫生物学相关。利用基因编辑进行的分析显著加深了对HGF-Met系统在基础生物学及其临床应用方面的深入理解。HGF和Met基因敲除(KO)小鼠在胚胎期致死。因此,为了研究HGF-Met信号通路的信号传导潜能,Met多功能对接位点中的氨基酸已被与下游衔接分子的特异性结合基序进行了交换。使用Cre-loxP方法构建了条件性Met基因敲除小鼠,对这些小鼠的特征分析表明,HGF-Met信号通路在各种组织类型和细胞的再生、保护和内环境稳定中至关重要。此外,使用HGF过表达小鼠的研究结果表明,HGF对各种类型的疾病和损伤具有治疗潜力。在本综述中,总结了基因编辑小鼠的表型。

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