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调节性T细胞在肝移植后免疫耐受和排斥反应中的关键作用:与肠道微生物群的相互作用

The Critical Role of Regulatory T Cells in Immune Tolerance and Rejection Following Liver Transplantation: Interactions With the Gut Microbiome.

作者信息

Lee Soon Kyu, Kwon Jung Hyun, Jang Jeong Won, Bae Si Hyun, Yoon Seung Kew, Jung Eun Sun, Choi Jong Young

机构信息

Division of Hepatology, Department of Internal Medicine, Incheon St. Mary's Hospital, College of Medicine, The Catholic University of Korea, Seoul, Republic of Korea.

The Catholic University Liver Research Center, College of Medicine, The Catholic University of Korea, Seoul, Republic of Korea.

出版信息

Transplantation. 2025 May 1;109(5):784-793. doi: 10.1097/TP.0000000000005220. Epub 2025 Apr 17.

Abstract

Liver transplantation (LT) is the ultimate treatment for patients with end-stage liver disease or early hepatocellular carcinoma. In the context of LT, because of the unique immunological characteristics of human liver allograft, 5%-20% of selected LT recipients can achieve operational tolerance. Nonetheless, there remains a risk of rejection in LT patients. Maintaining immune homeostasis is thus crucial for improving clinical outcomes in these patients. In mechanism, several immune cells, including dendritic cells, Kupffer cells, myeloid-derived suppressor cells, hepatic stellate cells, regulatory B cells, and CD4 + regulatory T cells (Treg), contribute to achieving tolerance following LT. In terms of Treg, it plays a role in successfully minimizing immunosuppression or achieving tolerance post-LT while also reducing the risk of rejection. Furthermore, the gut microbiome modulates systemic immune functions along the gut-liver axis. Recent studies have explored changes in the microbiome and its metabolites under various conditions, including post-LT, acute rejection, and tolerance. Certain functional microbiomes and metabolites exhibit immunomodulatory functions, such as the augmentation of Treg, influencing immune homeostasis. Therefore, understanding the mechanisms of tolerance in LT, the role of Treg in tolerance and rejection, as well as their interactions with gut microbiome, is vital for the management of LT patients.

摘要

肝移植(LT)是终末期肝病或早期肝细胞癌患者的最终治疗方法。在肝移植的背景下,由于人肝同种异体移植独特的免疫特性,5%-20%经过挑选的肝移植受者能够实现手术耐受。尽管如此,肝移植患者仍存在排斥反应的风险。因此,维持免疫稳态对于改善这些患者的临床结局至关重要。在机制方面,包括树突状细胞、库普弗细胞、髓源性抑制细胞、肝星状细胞、调节性B细胞和CD4 +调节性T细胞(Treg)在内的几种免疫细胞有助于肝移植后实现耐受。就Treg而言,它在成功最小化免疫抑制或肝移植后实现耐受的同时,还降低了排斥反应的风险。此外,肠道微生物群沿着肠-肝轴调节全身免疫功能。最近的研究探讨了包括肝移植后、急性排斥反应和耐受等各种情况下微生物群及其代谢产物的变化。某些功能性微生物群和代谢产物具有免疫调节功能,如增强Treg,影响免疫稳态。因此,了解肝移植耐受的机制、Treg在耐受和排斥反应中的作用以及它们与肠道微生物群的相互作用,对于肝移植患者的管理至关重要。

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