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四氯化碳诱导的大鼠肝纤维化中I、III和IV型胶原蛋白合成的动态变化及胶原生成细胞的分布

Dynamic changes of type I,III and IV collagen synthesis and distribution of collagen-producing cells in carbon tetrachloride-induced rat liver fibrosis.

作者信息

Du Wei-Dong, Zhang Yue-E, Zhai Wei-Rong, Zhou Xiao-Mei

出版信息

World J Gastroenterol. 1999 Oct;5(5):397-403. doi: 10.3748/wjg.v5.i5.397.

Abstract

AIM

To find out the relationship between the gene transcription of different types of procollagen and the deposition of the relevant collagens in the liver tissue and to confirm the types of collagen producing cells in liver fibrogenesis.METHODS:Dynamic changes of the expression of alpha1(I), alpha1(III) and alpha1(IV) procollagen mRNA and relevant collagens and the distribution of collagen producing cells during liver fibrogenesis of rat induced by CCl(4) (20 weeks) were investigated with Northern blot analysis, in situ hybridization and immunohistochemical techniques.RESULTS: The increased expression of alpha 1(III) procollagen mRNA by Northern blot analysis was the most predominant one among the three mRNAs during fibrogenesis. However, the enhanced expression of alpha1(IV) procollagen mRNA occurred very early while the expression of alpha1(I) mRNA was not enhanced much until the middle stage of the experiment. Desmin (Dm) positive hepatic stellate cells (HSCs) and few myofibroblasts (MFs) in and around the necrotic areas expressed alpha1(I), alpha1(III) and alpha1(IV) procollagen mRNA signals detected by in situ hybridization at the early stage of the experiment. All the three procollagen mRNA signals thereafter mainly localized in fibroblasts (Fbs) and MFs in fibrotic septa during the middle and late stages of fibrosis, which distributed parallel to the corresponding collagens detected by immunohistochemical study. In addition, the endothelial cells of sinusoids and the small blood vessels within the septa also showed alpha1(IV) procollagen mRNA and type IV collagen expression.CONCLUSION:It is considered that "HSC-MF-Fb effect cell system is the major cellular source of collagen production in liver fibrosis, in which HSCs are collagen producing precursor cells in the early liver fibrogenesis, thereafter the synthesis of type I, III and IV collagens (Col I, Col III and Col IV) mainly derives from MFs and Fbs, which play a very important role in the progress of liver fibrosis. The endothelial cells along sinusoids, as another source of Col IV production, might participate in the capillization of liver sinusoids.

摘要

目的

探讨不同类型前胶原基因转录与肝组织中相关胶原沉积之间的关系,并确定肝纤维化形成过程中胶原产生细胞的类型。方法:采用Northern印迹分析、原位杂交和免疫组化技术,研究四氯化碳诱导大鼠肝纤维化(20周)过程中α1(I)、α1(III)和α1(IV)前胶原mRNA及相关胶原表达的动态变化,以及胶原产生细胞的分布。结果:Northern印迹分析显示,在纤维化过程中,α1(III)前胶原mRNA表达增加最为显著。然而,α1(IV)前胶原mRNA的增强表达出现得非常早,而α1(I)mRNA直到实验中期才显著增强。实验早期,原位杂交检测到结蛋白(Dm)阳性的肝星状细胞(HSCs)以及坏死区域内和周围的少量肌成纤维细胞(MFs)表达α1(I)、α1(III)和α1(IV)前胶原mRNA信号。此后,在纤维化的中晚期,所有这三种前胶原mRNA信号主要定位于纤维间隔中的成纤维细胞(Fbs)和MFs,其分布与免疫组化研究检测到的相应胶原平行。此外,肝血窦内皮细胞和间隔内的小血管也显示出α1(IV)前胶原mRNA和IV型胶原表达。结论:认为“HSC-MF-Fb效应细胞系统”是肝纤维化中胶原产生的主要细胞来源,其中HSCs是肝纤维化早期的胶原产生前体细胞,此后I型、III型和IV型胶原(Col I、Col III和Col IV)的合成主要来源于MFs和Fbs,它们在肝纤维化进展中起非常重要的作用。沿肝血窦的内皮细胞作为Col IV产生的另一个来源,可能参与肝血窦的毛细血管化。

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