Department of Biomedicine, Centre for Cancer Biomarkers, University of Bergen, Bergen, Norway.
Institute of Biomedical Research of Barcelona (IIBB-CSIC), Institut d'Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS), Barcelona, Spain.
Front Immunol. 2024 May 16;15:1400553. doi: 10.3389/fimmu.2024.1400553. eCollection 2024.
Metabolic dysfunction-associated steatohepatitis (MASH) is a significant health concern with limited treatment options. AXL, a receptor tyrosine kinase activated by the GAS6 ligand, promotes MASH through activation of hepatic stellate cells and inflammatory macrophages. This study identified cell subsets affected by MASH progression and the effect of AXL inhibition.
Mice were fed chow or different fat-enriched diets to induce MASH, and small molecule AXL kinase inhibition with bemcentinib was evaluated. Gene expression was measured by qPCR. Time-of-flight mass cytometry (CyTOF) used single cells from dissociated livers, acquired on the Fluidigm Helios, and cell populations were studied using machine learning.
In mice fed different fat-enriched diets, liver steatosis alone was insufficient to elevate plasma soluble AXL (sAXL) levels. However, in conjunction with inflammation, sAXL increases, serving as an early indicator of steatohepatitis progression. Bemcentinib, an AXL inhibitor, effectively reduced proinflammatory responses in MASH models, even before fibrosis appearance. Utilizing CyTOF analysis, we detected a decreased population of Kupffer cells during MASH while promoting infiltration of monocytes/macrophages and CD8 T cells. Bemcentinib partially restored Kupffer cells, reduced pDCs and GzmB NK cells, and increased GzmBCD8 T cells and LSECs. Additionally, AXL inhibition enhanced a subtype of GzmBCD8 tissue-resident memory T cells characterized by CX3CR1 expression. Furthermore, bemcentinib altered the transcriptomic landscape associated with MASH progression, particularly in TLR signaling and inflammatory response, exhibiting differential cytokine expression in the plasma, consistent with liver repair and decreased inflammation.
Our findings highlight sAXL as a biomarker for monitoring MASH progression and demonstrate that AXL targeting shifted liver macrophages and CD8 T-cell subsets away from an inflammatory phenotype toward fibrotic resolution and organ healing, presenting a promising strategy for MASH treatment.
代谢相关脂肪性肝炎(MASH)是一种严重的健康问题,目前治疗选择有限。AXL 是一种受 GAS6 配体激活的受体酪氨酸激酶,通过激活肝星状细胞和炎症性巨噬细胞促进 MASH。本研究旨在确定受 MASH 进展影响的细胞亚群以及 AXL 抑制的作用。
用常规饲料或不同的高脂肪饮食喂养小鼠以诱导 MASH,并评估小分子 AXL 激酶抑制剂 bemcentinib 的作用。通过 qPCR 测量基因表达。利用来自分离肝脏的单细胞进行飞行时间质谱流式细胞术(CyTOF)分析,在 Fluidigm Helios 上获取数据,并使用机器学习研究细胞群体。
在喂食不同高脂肪饮食的小鼠中,单纯的肝脂肪变性不足以升高血浆可溶性 AXL(sAXL)水平。然而,与炎症结合时,sAXL 会增加,成为肝脂肪性肝炎进展的早期指标。AXL 抑制剂 bemcentinib 可有效降低 MASH 模型中的促炎反应,甚至在纤维化出现之前。利用 CyTOF 分析,我们在 MASH 过程中检测到库普弗细胞群体减少,同时促进单核细胞/巨噬细胞和 CD8 T 细胞浸润。Bemcentinib 部分恢复了库普弗细胞,减少了 pDC 和 GzmB NK 细胞,增加了 GzmBCD8 T 细胞和 LSEC。此外,AXL 抑制增强了一种表达 CX3CR1 的 GzmBCD8 组织驻留记忆 T 细胞亚型。此外,bemcentinib 改变了与 MASH 进展相关的转录组图谱,特别是在 TLR 信号和炎症反应中,血浆中差异表达的细胞因子与肝脏修复和炎症减轻一致。
我们的研究结果强调 sAXL 作为监测 MASH 进展的生物标志物,并表明 AXL 靶向作用将肝巨噬细胞和 CD8 T 细胞亚群从炎症表型转向纤维化消退和器官愈合,为 MASH 治疗提供了一种有前途的策略。
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