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Chemokines in liver inflammation and fibrosis.

机译:趋化因子在肝脏炎症和纤维化中的作用。

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摘要

Chemokines are a class of small chemotactic molecules with cytokine-like functions, which are well known to orchestrate inflammatory responses within different organs. Overall, more than 50 ligands and 19 receptors belong to the network. In recent years, accumulating functional and genetic evidence suggests that chemokines play a critical role in acute and chronic liver diseases, mediating the infiltration of immune cells (monocytes, T-cells) into the injured liver along a concentration gradient. However, chemokines can also directly affect the biology of liver resident cells, such as hepatic stellate cells and hepatocytes during inflammatory and fibrogenic tissue responses. Although the chemokine system has long been considered highly redundant, studies in knockout animals have convincingly demonstrated that single chemokines and chemokine receptors strongly affect the phenotype of toxic and inflammatory liver disease in vivo. However, depending on the model, these effects can be harmful (proinflammatory, profibrogenic) or beneficial (antifibrotic). This aspect of chemokine biology must be understood before these molecules and their receptors are targeted for therapeutic purposes. Here, we summarize current knowledge on the genetic and functional importance of the chemokine network in injury and highlight their potential for intervening in the inflammation and fibrosis that drives liver disease progression.
机译:趋化因子是一类具有细胞因子样功能的小趋化分子,众所周知,它能协调不同器官内的炎症反应。总体而言,该网络包含50多个配体和19个受体。近年来,越来越多的功能和遗传证据表明趋化因子在急性和慢性肝病中起着至关重要的作用,其介导免疫细胞(单核细胞,T细胞)沿浓度梯度渗入受伤的肝脏。然而,趋化因子还可以在炎症和纤维化组织反应过程中直接影响肝脏驻留细胞的生物学,例如肝星状细胞和肝细胞。尽管长期以来一直认为趋化因子系统是高度冗余的,但在基因敲除动物中的研究已令人信服地表明,单个趋化因子和趋化因子受体在体内强烈影响毒性和炎症性肝病的表型。但是,根据模型的不同,这些作用可能是有害的(促炎性,促纤维化的)或有益的(抗纤维化的)。在靶向这些分子及其受体以达到治疗目的之前,必须先了解趋化因子生物学的这一方面。在这里,我们总结了趋化因子网络在损伤中的遗传和功能重要性方面的当前知识,并着重指出了它们可能干预驱动肝病进展的炎症和纤维化。

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