Du Hui-Juan, Zhao Su-Xian, Zhao Wen, Fu Na, Li Wen-Cong, Qin Xiao-Jie, Zhang Yu-Guo, Nan Yue-Min, Zhao Jing-Min
Department of Traditional and Western Medical Hepatology, the Third Hospital of Hebei Medical University, Shijiazhuang, Hebei, China.
Department of Pathology and Hepatology Institution, The Fifth Medical Center, General Hospital of PLA, Beijing, China.
Histol Histopathol. 2021 Jun;36(6):653-662. doi: 10.14670/HH-18-340. Epub 2021 Apr 15.
Inflammatory activation of hepatic macrophages plays a primary role in drug-induced liver injury (DILI). However, the exact mechanism underlying DILI remains unclear.
A total of 328 DILI patients and 80 healthy individuals were prospectively enrolled in this study. The DILI patients were categorized into subgroups based on either disease severity or histopathological patterns. Plasma soluble CD163 (sCD163) and hepatic CD163 were examined to determine hepatic macrophage activation, and CD8, CD20, and MUM-1 were assessed to determine cellular immunity using immunohistochemistry. The lipopolysaccharide (LPS) pathway proteins [e.g. LPS, soluble CD14 (sCD14), and LPS-binding protein (LBP)] were measured using enzyme-linked immunosorbent assay.
Plasma sCD163 levels were nine-fold higher in DILI patients than in healthy controls at the baseline, but significantly decreased at the 4-week follow-up visit after treatment. The numbers of hepatic macrophages, B cells, and plasma cells were significantly higher in the liver tissues from DILI patients than those from healthy controls. Furthermore, the baseline levels of LPS pathway proteins in the DILI patients were significantly higher than those in the controls. Notably, these proteins significantly decreased at the 4-week follow-up visit but remained significantly higher than the levels for the controls.
Hepatic inflammation in DILI involves the activation of hepatic macrophages and cellular immunity, in which the LPS pathway likely plays a role, at least in part. As such, this study has improved our understanding of the pathological mechanisms for DILI and may facilitate the development of better treatments for patients with DILI.
肝巨噬细胞的炎症激活在药物性肝损伤(DILI)中起主要作用。然而,DILI的确切机制仍不清楚。
本研究前瞻性纳入了328例DILI患者和80名健康个体。根据疾病严重程度或组织病理学模式将DILI患者分为亚组。检测血浆可溶性CD163(sCD163)和肝脏CD163以确定肝巨噬细胞的激活情况,并使用免疫组织化学评估CD8、CD20和MUM-1以确定细胞免疫。使用酶联免疫吸附测定法测量脂多糖(LPS)途径蛋白[如LPS、可溶性CD14(sCD14)和LPS结合蛋白(LBP)]。
在基线时,DILI患者的血浆sCD163水平比健康对照高9倍,但在治疗后的4周随访时显著降低。DILI患者肝组织中的肝巨噬细胞、B细胞和浆细胞数量显著高于健康对照。此外,DILI患者中LPS途径蛋白的基线水平显著高于对照。值得注意的是,这些蛋白在4周随访时显著降低,但仍显著高于对照水平。
DILI中的肝脏炎症涉及肝巨噬细胞的激活和细胞免疫,其中LPS途径可能至少部分发挥作用。因此,本研究增进了我们对DILI病理机制的理解,并可能有助于为DILI患者开发更好的治疗方法。
