o-11 增强肝组织中的 f4/80+cd11b-cd206+ kupffer 细胞:作为保肝剂的马钱子素-1 的作用

IF 3.7 3区 医学 Q2 GASTROENTEROLOGY & HEPATOLOGY
Jessica Zuñiga , Andres Herrada , Francisca Herrera , Alexandra Olate
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引用次数: 0

摘要

导言和目的慢性肝病(CLD)是全球主要的健康负担,是全球第11大死因和第15大发病原因。慢性肝病可能伴有脂肪变性和肝纤维化,并发展为肝硬化,同时伴有肝功能衰竭。目前,还没有获得批准的治疗方法,只建议消除致病因子或进行姑息治疗。免疫反应,尤其是肝巨噬细胞(Kupffer 细胞),在肝病的发展中起着根本性的作用。众所周知,肝脏中同时存在分化良好的群体,包括F4/80+CD11b-(无柄)和 F4/80+CD11b+(从骨髓移入)。这些种群可将其表型从 M1(炎症性)转变为 M2(抗炎症性),而这正是药理学所关注的。我们的目的是研究 Maresin-1(一种欧米伽-3 脂肪酸的衍生物)是否能通过增加 CD206+CD86-CD11c- 即 M2 Kupffer 细胞群来促进恢复状态。分离肝脏巨噬细胞:进行实时 qPCR 流式细胞分析和细胞测定。结果服用 MaR1 改变了 Kupffer 细胞群,使 M2 F4/80+CD11b-CD206+ 和 F4/80intCD11b+CD206+ 亚群增加,CD86+CD11c+ 亚群减少。结论综上所述,这些结果表明 Mar1 可使 Kupffer 细胞转向抗炎、恢复和修复状态,从而起到保肝作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
O-11 ENHANCEMENT OF F4/80+CD11B-CD206+ KUPFFER CELLS IN LIVER TISSUE: EFFECT OF MARESIN-1 AS HEPATOPROTECTIVE AGENT

Introduction and Objectives

Chronic liver diseases (CLD) are a major global health burden and are the 11th leading cause of death and the 15th cause of morbidity worldwide. CLD could be associated with steatosis and fibrosis and progress to cirrhosis, with the concomitant liver failure. Currently, there is no approved treatment and it is only recommended to eliminate the causative agent or give palliative treatments. The immune response, particularly hepatic macrophages (Kupffer cells), play a fundamental role in the development of liver disease. It is known that well-differentiated populations coexist in the liver, including: F4/80+CD11b- (sessile) and F4/80+CD11b+ (migrated from bone marrow). These populations could be modified their phenotype from M1 (inflammatory) to M2 (anti-inflammatory), which is of pharmacological interest. We aimed to study the administration of Maresin-1, a derivative of omega-3 fatty acids, promote a restorative state by an increase in the CD206+CD86-CD11c- i.e. M2 Kupffer cell population.

Materials and Methods

male C57bl/c mice were subjected to liver fibrosis by i.p diethylnitrosamine (DEN) 50 mg/kg twice a week and treated with MaR1 (4ng/g) for 9 weeks. The liver macrophages were isolated: real-time qPCR flow and cytometry were made. In addition, MaR1 was administered to healthy mice to observe the role MaR1 on hepatic macrophage populations.

Results

The administration of MaR1 modifies the Kupffer cells populations, generating an increase in the subpopulations of M2 F4/80+CD11b-CD206+ and F4/80intCD11b+CD206+, with a decrease in the CD86+CD11c+, both in the fibrosis as in healthy mice. This was accompanied by an increase in IL-10 cytokines and a fall in TNF-a values.

Conclusions

Taken together, these results indicate that Mar1 switches the Kupffer cells towards an anti-inflammatory, restorative and resolving state, acting as a hepatoprotective agent.

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来源期刊
Annals of hepatology
Annals of hepatology 医学-胃肠肝病学
CiteScore
7.90
自引率
2.60%
发文量
183
审稿时长
4-8 weeks
期刊介绍: Annals of Hepatology publishes original research on the biology and diseases of the liver in both humans and experimental models. Contributions may be submitted as regular articles. The journal also publishes concise reviews of both basic and clinical topics.
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