Trovato Francesca M, Zia Rabiya, Napoli Salvatore, Wolfer Kate, Huang Xiaohong, Morgan Phillip E, Husbyn Hannah, Elgosbi Marwa, Lucangeli Manuele, Miquel Rosa, Wilson Ian, Heaton Nigel David, Heneghan Michael A, Auzinger Georg, Antoniades Charalambos G, Wendon Julia A, Patel Vishal C, Coen Muireann, Triantafyllou Evangelos, McPhail Mark J
Department of Inflammation BiologySchool of Immunity and Microbial SciencesKings College LondonUK.
Institute of Liver StudiesKings College HospitalLondonUK.
Hepatology. 2021 Aug;74(2):907-925. doi: 10.1002/hep.31738. Epub 2021 Jun 15.
BACKGROUND & AIMS: Acute-on-chronic liver failure (ACLF) is characterized by systemic inflammation, monocyte dysfunction, and susceptibility to infection. Lysophosphatidylcholines (LPCs) are immune-active lipids whose metabolic regulation and effect on monocyte function in ACLF is open for study.
APPROACHES & RESULTS: Three hundred forty-two subjects were recruited and characterized for blood lipid, cytokines, phospholipase (PLA), and autotaxin (ATX) concentration. Peripheral blood mononuclear cells and CD14 monocytes were cultured with LPC, or its autotaxin (ATX)-derived product, lysophosphatidic acid (LPA), with or without lipopolysaccharide stimulation and assessed for surface marker phenotype, cytokines production, ATX and LPA-receptor expression, and phagocytosis. Hepatic ATX expression was determined by immunohistochemistry. Healthy volunteers and patients with sepsis or acute liver failure served as controls. ACLF serum was depleted in LPCs with up-regulated LPA levels. Patients who died had lower LPC levels than survivors (area under the receiver operating characteristic curve, 0.94; P < 0.001). Patients with high-grade ACLF had the lowest LPC concentrations and these rose over the first 3 days of admission. ATX concentrations were higher in patients with AD and ACLF and correlated with Model for End-Stage Liver Disease, Consortium on Chronic Liver Failure-Sequential Organ Failure Assessment, and LPC/LPA concentrations. Reduction in LPC correlated with higher monocyte Mer-tyrosine-kinase (MerTK) and CD163 expression. Plasma ATX concentrations rose dynamically during ACLF evolution, correlating with IL-6 and TNF-α, and were associated with increased hepatocyte ATX expression. ACLF patients had lower human leukocyte antigen-DR isotype and higher CD163/MerTK monocyte expression than controls; both CD163/MerTK expression levels were reduced in ACLF ex vivo following LPA, but not LPC, treatment. LPA induced up-regulation of proinflammatory cytokines by CD14 cells without increasing phagocytic capacity.
ATX up-regulation in ACLF promotes LPA production from LPC. LPA suppresses MerTK/CD163 expression and increases monocyte proinflammatory cytokine production. This metabolic pathway could be investigated to therapeutically reprogram monocytes in ACLF.
慢加急性肝衰竭(ACLF)的特征为全身炎症反应、单核细胞功能障碍及易感性感染。溶血磷脂酰胆碱(LPC)是具有免疫活性的脂质,其在ACLF中的代谢调控及其对单核细胞功能的影响尚待研究。
招募342名受试者,测定其血脂、细胞因子、磷脂酶(PLA)及自分泌运动因子(ATX)浓度。外周血单个核细胞和CD14单核细胞分别与LPC或其由ATX衍生的产物溶血磷脂酸(LPA)共同培养,有无脂多糖刺激,评估细胞表面标志物表型、细胞因子产生、ATX及LPA受体表达和吞噬作用。通过免疫组化测定肝脏ATX表达。健康志愿者及脓毒症或急性肝衰竭患者作为对照。ACLF患者血清中LPC水平降低,LPA水平上调。死亡患者的LPC水平低于存活者(受试者工作特征曲线下面积为0.94;P < 0.001)。重度ACLF患者的LPC浓度最低,且在入院后的头3天有所上升。AD和ACLF患者的ATX浓度较高,且与终末期肝病模型、慢性肝衰竭-序贯器官衰竭评估联合会及LPC/LPA浓度相关。LPC降低与单核细胞Mer-酪氨酸激酶(MerTK)及CD163表达升高相关。在ACLF进展过程中,血浆ATX浓度动态升高,与白细胞介素-6和肿瘤坏死因子-α相关,并与肝细胞ATX表达增加有关。与对照组相比,ACLF患者的人类白细胞抗原-DR同种型较低,CD163/MerTK单核细胞表达较高;LPA而非LPC处理后,ACLF患者离体培养的细胞中CD163/MerTK表达水平均降低。LPA诱导CD14细胞促炎细胞因子上调,但不增加吞噬能力。
ACLF中ATX上调促进LPC生成LPA。LPA抑制MerTK/CD163表达并增加单核细胞促炎细胞因子产生。可研究该代谢途径以对ACLF中的单核细胞进行治疗性重编程。
