Kim Jieun, Wang Sihyung, Lee Chanbin, Sung Sumi, Shin Yongbo, Song Kyoung Seob, Cha Hee-Jae, Ock Meesun, Jung Youngmi
Department of Integrated Biological Science, College of Natural Science, Pusan National University, Pusan, Republic of Korea.
Department of Physiology, Kosin University College of Medicine, Pusan, Republic of Korea.
Cell Physiol Biochem. 2018;50(4):1414-1428. doi: 10.1159/000494604. Epub 2018 Oct 24.
BACKGROUND/AIMS: Malaria is the most deadly parasitic infection in the world, resulting in damage to various organs, including the liver, of the infected organism; however, the mechanism causing this damage in the liver remains unclear. Liver fibrosis, a major characteristic of liver diseases, occurs in response to liver injury and is regulated by a complex network of signaling pathways. Hedgehog (Hh) signaling orchestrates a number of hepatic responses including hepatic fibrogenesis. Therefore, we investigated whether Hh signaling influenced the liver's response to malarial infection.
Eight-week-old male C57BL/6 mice inoculated with blood containing Plasmodium berghei ANKA (PbA)-infected erythrocytes were sacrificed when the level of parasitemia in the blood reached 10% or 30%, and the livers were collected for biochemical analysis. Liver responses to PbA infection were examined by hematoxylin and eosin staining, real-time polymerase chain reaction, immunohistochemistry and western blot.
Severe hepatic injury, such as ballooned hepatocytes, sinusoidal dilatation, and infiltrated leukocytes, was evident in the livers of the malaria-infected mice. Hypoxia was also induced in 30% parasitemia group. With the accumulation of Kupffer cells, inflammation markers, TNF-α, interleukin-1β, and chemokine (C-X-C motif) ligand 1, were significantly upregulated in the infected group compared with the control group. Expression of fibrotic markers, including transforming growth factor-β, α-smooth muscle actin (α-SMA), collagen 1a1, thymosin β4, and vimentin, were significantly higher in the infected groups than in the control group. With increased collagen deposition, hepatic stellate cells expressing α-SMA accumulated in the liver of the PbA-infected mice, whereas those cells were rarely detected in the livers of the control mice. The levels of Hh signaling and Yes-associated protein (YAP), two key regulators for hepatic fibrogenesis, were significantly elevated in the infected groups compared with the control group. Treatment of mice with Hh inhibitor, GDC-0449, reduced hepatic inflammation and fibrogenesis with Hh suppression in PbA-infected mice.
Our results demonstrate that HSCs are activated in and Hh and YAP signaling are associated with this process, contributing to increased hepatic fibrosis in malaria-infected livers.
背景/目的:疟疾是世界上最致命的寄生虫感染,会对受感染机体的各种器官造成损害,包括肝脏;然而,肝脏中导致这种损害的机制仍不清楚。肝纤维化是肝脏疾病的一个主要特征,它是对肝损伤的反应,由复杂的信号通路网络调节。刺猬信号通路(Hh)协调包括肝纤维化形成在内的多种肝脏反应。因此,我们研究了Hh信号通路是否影响肝脏对疟疾感染的反应。
当血液中疟原虫血症水平达到10%或30%时,处死接种含有感染伯氏疟原虫ANKA(PbA)红细胞血液的8周龄雄性C57BL/6小鼠,并收集肝脏进行生化分析。通过苏木精和伊红染色、实时聚合酶链反应、免疫组织化学和蛋白质印迹法检测肝脏对PbA感染的反应。
在疟疾感染小鼠的肝脏中,明显出现严重的肝损伤,如肝细胞气球样变、窦状隙扩张和白细胞浸润。在疟原虫血症为30%的组中也诱导了缺氧。随着库普弗细胞的积累,与对照组相比,感染组中炎症标志物肿瘤坏死因子-α、白细胞介素-1β和趋化因子(C-X-C基序)配体1显著上调。包括转化生长因子-β、α-平滑肌肌动蛋白(α-SMA)、胶原蛋白1a1、胸腺素β4和波形蛋白在内的纤维化标志物的表达在感染组中显著高于对照组。随着胶原蛋白沉积增加,表达α-SMA的肝星状细胞在PbA感染小鼠的肝脏中积聚,而在对照小鼠的肝脏中很少检测到这些细胞。与对照组相比,感染组中肝纤维化形成的两个关键调节因子Hh信号通路和Yes相关蛋白(YAP)的水平显著升高。用Hh抑制剂GDC-0449处理小鼠可减轻PbA感染小鼠的肝脏炎症和纤维化,并抑制Hh。
我们的结果表明,在疟疾感染的肝脏中肝星状细胞被激活,Hh和YAP信号通路与这一过程相关,导致肝纤维化增加。
Zotero 插件