Age-dependent development of liver fibrosis in Glmp (gt/gt) mice.

Fibrogenesis & Tissue Repair Pub Date : 2016-04-28 eCollection Date: 2016-01-01 DOI:10.1186/s13069-016-0042-4
Cecilie K Nesset, Xiang Yi Kong, Markus Damme, Camilla Schjalm, Norbert Roos, Else Marit Løberg, Winnie Eskild
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引用次数: 6

Abstract

Background: Mice lacking glycosylated lysosomal membrane protein (Glmp (gt/gt) mice) have liver fibrosis as the predominant phenotype due to chronic liver injury. The Glmp (gt/gt) mice grow and reproduce at the same rate as their wild-type siblings. Life expectancy is around 18 months.

Methods: Wild-type and Glmp (gt/gt) mice were studied between 1 week and 18 months of age. Livers were analyzed using histological, immunohistochemical, biochemical, and qPCR analyses.

Results: It was shown that Glmp (gt/gt) mice were not born with liver injury; however, it appeared shortly after birth as indicated by excess collagen expression, deposition of fibrous collagen in the periportal areas, and increased levels of hydroxyproline in Glmp (gt/gt) liver. Liver functional tests indicated a chronic, mild liver injury. Markers of inflammation, fibrosis, apoptosis, and modulation of extracellular matrix increased from an early age, peaking around 4 months of age and followed by attenuation of these signals. To compensate for loss of hepatocytes, the oval cell compartment was activated, with the highest activity of the oval cells detected at 3 months of age, suggesting insufficient hepatocyte proliferation in Glmp (gt/gt) mice around this age. Although constant proliferation of hepatocytes and oval cells maintained adequate hepatic function in Glmp (gt/gt) mice, it also resulted in a higher frequency of liver tumors in older animals.

Conclusions: The Glmp (gt/gt) mouse is proposed as a model for slowly progressing liver fibrosis and possibly as a model for a yet undescribed human lysosomal disorder.

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Glmp (gt/gt)小鼠肝纤维化的年龄依赖性发展。
背景:缺乏糖基化溶酶体膜蛋白的小鼠(Glmp (gt/gt)小鼠)由于慢性肝损伤导致肝纤维化为主要表型。Glmp (gt/gt)小鼠的生长和繁殖速度与它们的野生型兄弟姐妹相同。预期寿命在18个月左右。方法:以野生型和Glmp (gt/gt)小鼠为研究对象,年龄为1周龄~ 18月龄。采用组织学、免疫组织化学、生化和qPCR分析肝脏。结果:Glmp (gt/gt)小鼠出生时无肝损伤;然而,它在出生后不久就出现了,表现为胶原表达过剩,纤维胶原沉积在门静脉周围区域,Glmp (gt/gt)肝脏中羟脯氨酸水平升高。肝功能检查显示慢性轻度肝损伤炎症、纤维化、细胞凋亡和细胞外基质调节的标志物从早期开始增加,在4个月左右达到峰值,随后这些信号减弱。为了弥补肝细胞的损失,卵形细胞室被激活,在3个月大时检测到卵形细胞的最高活性,表明在这个年龄的Glmp (gt/gt)小鼠肝细胞增殖不足。虽然Glmp (gt/gt)小鼠肝细胞和卵圆细胞的持续增殖维持了足够的肝功能,但它也导致老年动物肝脏肿瘤的频率更高。结论:Glmp (gt/gt)小鼠被认为是缓慢进展性肝纤维化的模型,也可能是尚未描述的人类溶酶体疾病的模型。
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Matrix and cell phenotype differences in Dupuytren's disease. Activation of hepatic stellate cell in Pten null liver injury model. Protective role for miR-9-5p in the fibrogenic transformation of human dermal fibroblasts. Age-dependent development of liver fibrosis in Glmp (gt/gt) mice. Active transforming growth factor-β is associated with phenotypic changes in granulomas after drug treatment in pulmonary tuberculosis.
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