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循环免疫细胞中独特的免疫代谢特征决定了慢加急性肝衰竭的疾病转归。

Distinct immunometabolic signatures in circulating immune cells define disease outcome in acute-on-chronic liver failure.

作者信息

Feio-Azevedo Rita, Boesch Markus, Radenkovic Silvia, van Melkebeke Lukas, Smets Lena, Wallays Marie, Boeckx Bram, Philips Gino, Prata de Oliveira Janaíne, Ghorbani Mohammad, Laleman Wim, Meersseman Philippe, Wilmer Alexander, Cassiman David, van Malenstein Hannah, Triantafyllou Evangelos, Sánchez Cristina, Aguilar Ferran, Nevens Frederik, Verbeek Jef, Moreau Richard, Arroyo Vicente, Denadai Souza Alexandre, Clària Joan, Lambrechts Diether, Ghesquière Bart, Korf Hannelie, van der Merwe Schalk

机构信息

Laboratory of Hepatology, CHROMETA Department, KU Leuven, Leuven, Belgium.

Metabolomics Expertise Center, Center for Cancer Biology, VIB Center for Cancer Biology, Leuven, Belgium.

出版信息

Hepatology. 2025 Feb 1;81(2):509-522. doi: 10.1097/HEP.0000000000000907. Epub 2024 May 16.

DOI:10.1097/HEP.0000000000000907
PMID:38761406
原文链接:
https://pmc.ncbi.nlm.nih.gov/articles/PMC11737128/
Abstract

BACKGROUND AND AIMS

Acute-on-chronic liver failure (ACLF) is a complication of cirrhosis characterized by multiple organ failure and high short-term mortality. The pathophysiology of ACLF involves elevated systemic inflammation leading to organ failure, along with immune dysfunction that heightens susceptibility to bacterial infections. However, it is unclear how these aspects are associated with recovery and nonrecovery in ACLF.

APPROACH AND RESULTS

Here, we mapped the single-cell transcriptome of circulating immune cells from patients with ACLF and acute decompensated (AD) cirrhosis and healthy individuals. We further interrogate how these findings, as well as immunometabolic and functional profiles, associate with ACLF-recovery (ACLF-R) or nonrecovery (ACLF-NR). Our analysis unveiled 2 distinct states of classical monocytes (cMons). Hereto, ACLF-R cMons were characterized by transcripts associated with immune and stress tolerance, including anti-inflammatory genes such as RETN and LGALS1 . Additional metabolomic and functional validation experiments implicated an elevated oxidative phosphorylation metabolic program as well as an impaired ACLF-R cMon functionality. Interestingly, we observed a common stress-induced tolerant state, oxidative phosphorylation program, and blunted activation among lymphoid populations in patients with ACLF-R. Conversely, ACLF-NR cMon featured elevated expression of inflammatory and stress response genes such as VIM , LGALS2 , and TREM1 , along with blunted metabolic activity and increased functionality.

CONCLUSIONS

This study identifies distinct immunometabolic cellular states that contribute to disease outcomes in patients with ACLF. Our findings provide valuable insights into the pathogenesis of ACLF, shedding light on factors driving either recovery or nonrecovery phenotypes, which may be harnessed as potential therapeutic targets in the future.

摘要

背景与目的

慢加急性肝衰竭(ACLF)是肝硬化的一种并发症,其特征为多器官功能衰竭及短期高死亡率。ACLF的病理生理学涉及全身炎症反应增强导致器官功能衰竭,以及免疫功能障碍,这会增加细菌感染的易感性。然而,目前尚不清楚这些方面与ACLF患者的恢复和未恢复情况如何相关。

方法与结果

在此,我们绘制了ACLF患者、急性失代偿(AD)肝硬化患者及健康个体循环免疫细胞的单细胞转录组图谱。我们进一步探究这些发现以及免疫代谢和功能谱如何与ACLF恢复(ACLF-R)或未恢复(ACLF-NR)相关。我们的分析揭示了经典单核细胞(cMons)的两种不同状态。在此,ACLF-R cMons的特征是与免疫和应激耐受相关的转录本,包括抗炎基因如RETN和LGALS1。额外的代谢组学和功能验证实验表明氧化磷酸化代谢程序增强以及ACLF-R cMons功能受损。有趣的是,我们在ACLF-R患者的淋巴细胞群体中观察到一种共同的应激诱导耐受状态、氧化磷酸化程序以及激活减弱。相反,ACLF-NR cMons的特征是炎症和应激反应基因如VIM、LGALS2和TREM1的表达升高,同时代谢活性减弱且功能增强。

结论

本研究确定了不同的免疫代谢细胞状态,这些状态导致了ACLF患者的疾病结局。我们的发现为ACLF的发病机制提供了有价值的见解,揭示了驱动恢复或未恢复表型的因素,这些因素未来可能被用作潜在的治疗靶点。

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