MicroRNA-181b promotes schistosomiasis-induced hepatic fibrosis by targeting Smad7

IF 1.4 4区 医学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY Molecular and biochemical parasitology Pub Date : 2022-11-01 DOI:10.1016/j.molbiopara.2022.111523
Shu Wang , Jianqiang Zhang , Hui Chen , Xiang Zhan , Hao Nie , Chao Wang , Yanxiang Zhang , Bing Zheng , Quan Gong
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引用次数: 1

Abstract

Schistosomiasis is a common parasitic disease. Hepatosplenic schistosomiasis, caused by Schistosoma japonicum and Schistosoma mansoni, involves pathological changes, including worm egg-induced hepatic granuloma and fibrosis, which can markedly affect the liver’s physiological functions. Although the drug praziquantel (PZQ) is used to treat schistosomiasis, drugs against schistosomiasis-induced liver fibrosis are rare in the clinical setting. Therefore, developing effective strategies to prevent and treat schistosomiasis-induced liver fibrosis is crucial. Previous studies have shown that miRNAs are involved in various liver diseases. In this study, we found a gradual increase in miR-181b expression in the murine liver as S. japonicum infection progressed, while the expression of Smad7 decreased. Down-regulating miR-181b significantly alleviated S. japonicum-induced hepatic granuloma and liver fibrosis. In vitro experiments showed that treatment with TGF-β1 upregulated miR-181b levels in the hepatic stellate cell (HSC) line LX2 in a concentration- and time-dependent manner. Downregulation of miR-181b significantly decreased collagen type I alpha 1 chain (COL1A1) expression in TGF-β1-stimulated LX2 cells. These findings indicate that miR-181b promotes HSC activation by down-regulating Smad7 expression, activating the TGF-β1/Smad signaling pathway, and leading to excess collagen expression and deposition. Our findings suggest that miR-181b might be a potentially novel therapeutic target for schistosomiasis-induced liver fibrosis.

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MicroRNA-181b通过靶向Smad7促进血吸虫病诱导的肝纤维化
血吸虫病是一种常见的寄生虫病。肝脾血吸虫病是由日本血吸虫和曼氏血吸虫引起的肝脾血吸虫病,其病理变化包括虫卵诱导的肝脏肉芽肿和纤维化,可明显影响肝脏的生理功能。尽管吡喹酮(PZQ)药物用于治疗血吸虫病,但临床上用于治疗血吸虫病引起的肝纤维化的药物很少。因此,制定有效的策略来预防和治疗血吸虫病引起的肝纤维化至关重要。先前的研究表明,mirna参与了多种肝脏疾病。在本研究中,我们发现随着日本血吸虫感染的进展,小鼠肝脏中miR-181b的表达逐渐增加,而Smad7的表达则下降。下调miR-181b可显著缓解日本血吸虫诱导的肝肉芽肿和肝纤维化。体外实验表明,TGF-β1处理可使肝星状细胞(HSC)系LX2中miR-181b水平呈浓度依赖性和时间依赖性上调。下调miR-181b可显著降低TGF-β1刺激的LX2细胞中胶原I型α 1链(COL1A1)表达。这些发现表明,miR-181b通过下调Smad7表达,激活TGF-β1/Smad信号通路,导致胶原过度表达和沉积,从而促进HSC活化。我们的研究结果表明,miR-181b可能是血吸虫病诱导肝纤维化的潜在新治疗靶点。
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来源期刊
CiteScore
2.90
自引率
0.00%
发文量
51
审稿时长
63 days
期刊介绍: The journal provides a medium for rapid publication of investigations of the molecular biology and biochemistry of parasitic protozoa and helminths and their interactions with both the definitive and intermediate host. The main subject areas covered are: • the structure, biosynthesis, degradation, properties and function of DNA, RNA, proteins, lipids, carbohydrates and small molecular-weight substances • intermediary metabolism and bioenergetics • drug target characterization and the mode of action of antiparasitic drugs • molecular and biochemical aspects of membrane structure and function • host-parasite relationships that focus on the parasite, particularly as related to specific parasite molecules. • analysis of genes and genome structure, function and expression • analysis of variation in parasite populations relevant to genetic exchange, pathogenesis, drug and vaccine target characterization, and drug resistance. • parasite protein trafficking, organelle biogenesis, and cellular structure especially with reference to the roles of specific molecules • parasite programmed cell death, development, and cell division at the molecular level.
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