TREM2 通过 SHP1/BTK 轴抑制脂肪酸氧化,从而加重败血症。

Siqi Ming,Xingyu Li,Qiang Xiao,Siying Qu,Qiaohua Wang,Qiongyan Fang,Pingping Liang,Yating Xu,Jingwen Yang,Yongqiang Yang,Xi Huang,Yongjian Wu
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摘要

脓毒症患者的脂肪酸氧化(FAO)功能受损,恢复 FAO 有助于治疗。然而,导致脓毒症期间脂肪酸氧化功能障碍的调节因素仍未得到充分阐明。在这项研究中,我们发现了以髓系细胞上表达的触发受体 2(TREM2)高表达为特征的脂质相关巨噬细胞亚群,并证明 TREM2 可抑制 FAO,从而增加对脓毒症的易感性。TREM2在败血症患者中的表达明显上调,并与败血症的严重程度相关。敲除巨噬细胞中的TREM2可提高脓毒症小鼠的存活率,减少炎症和器官损伤。值得注意的是,TREM2缺陷小鼠的甘油三酯积累减少,FAO率提高。进一步观察表明,阻断FAO大大缓解了TREM2基因敲除小鼠的症状。从机理上讲,我们证实 TREM2 与磷酸酶 SHP1 相互作用,抑制了脓毒症中布鲁顿酪氨酸激酶(BTK)介导的 FAO。我们的研究结果拓展了对脓毒症中FAO功能障碍的认识,并揭示了TREM2是FAO的一个关键调节因子,它可能为脓毒症的临床治疗提供一个有前景的靶点。
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TREM2 aggravates sepsis by inhibiting fatty acid oxidation via the SHP1/BTK axis.
Impaired fatty acid oxidation (FAO) and the therapeutic benefits of FAO restoration have been revealed in sepsis. However, the regulatory factors contributing to FAO dysfunction during sepsis remain inadequately clarified. In this study, we identified a subset of lipid-associated macrophages characterized by high expression of trigger receptor expressed on myeloid cells 2 (TREM2) and demonstrated that TREM2 acted as a suppressor of FAO to increase the susceptibility to sepsis. TREM2 expression was markedly up-regulated in sepsis patients and correlated with the severity of sepsis. Knock out of TREM2 in macrophages improved the survival rate and reduced inflammation and organ injuries of sepsis mice. Notably, TREM2-deficient mice exhibited decreased triglyceride accumulation and an enhanced FAO rate. Further observations showed that the blockade of FAO substantially abolished the alleviated symptoms observed in TREM2 knockout mice. Mechanically, we demonstrated that TREM2 interacted with the phosphatase SHP1 to inhibit Bruton tyrosine kinas (BTK)-mediated FAO in sepsis. Our findings expand the understanding of FAO dysfunction in sepsis and reveal TREM2 as a critical regulator of FAO, which may provide a promising target for the clinical treatment of sepsis.
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