Lund Laursen Tea, Brøckner Siggard Cecilie, Kazankov Konstantin, Damgaard Sandahl Thomas, Møller Holger Jon, Ong Adrian, Douglas Mark W, George Jacob, Tarp Britta, Hagelskjaer Kristensen Lena, Lund Laursen Alex, Hiramatsu Akira, Nakahara Takashi, Chayama Kazuaki, Grønbaek Henning
a Department of Hepatology & Gastroenterology , Aarhus University Hospital , Aarhus , Denmark.
b Department of Clinical Biochemistry , Aarhus University Hospital , Aarhus , Denmark.
Scand J Gastroenterol. 2018 Aug;53(8):986-993. doi: 10.1080/00365521.2018.1481996. Epub 2018 Jul 10.
Soluble CD 163 (sCD163) is released from activated liver macrophages in chronic viral hepatitis C (HCV) and serum levels reflect liver disease severity. The impact of direct-acting antiviral (DAA)-therapy on sCD163-levels and the ability of sCD163 to predict the presence of liver fibrosis remain unclear. In a combined observational and prospective study, we aimed to investigate changes in sCD163 with DAA-treatment, to investigate associations between sCD163 and histopathological activity and fibrosis and to validate the sCD163-based fibrosis score in HCV-patients.
We examined three groups of patients: an Australian (n = 28) treated with pegylated-interferon and a first-generation DAA, a Danish (n = 38) treated with sofosbuvir-based DAA-regimens and a Japanese (n = 562) assessed for activity and fibrosis (Metavir scoring system) in liver biopsies. Serum sCD163-levels were quantified by ELISA.
Thirteen (46%) of the Australian patients achieved sustained virological response (SVR) and only these patients had significant decreases in sCD163-levels (2.7 (95%CI:1.9-3.6) vs. 4.1(2.9-5.7) mg L , p = .008). In the Danish group, 37 (97%) patients achieved SVR at 12-weeks post-treatment with 32% reduction in sCD163-levels (5.0 (4.3-5.8) vs. 7.4 (6.3-8.7), p < .001). The decline was rapid and persisted 12 months after treatment cessation (p < .007). sCD163 levels increased in parallel with inflammatory activity and fibrosis (p < .001). The sCD163-based fibrosis score outperformed established fibrosis scores for significant fibrosis (areas under the receiver operating characteristics curves (AUROCs): 0.79 (0.75-0.83) vs. aspartate aminotransferase to platelet ratio index (APRI) 0.73 (0.69-0.77), Fibrosis-4 (FIB-4) 0.74 (0.70-0.78), p < .001).
sCD163-levels decline rapidly with successful DAA therapy and are associated with histological inflammatory activity and fibrosis, confirming a key role for macrophages in HCV inflammation and fibrosis and supporting sCD163 as a biomarker of treatment response.
可溶性CD163(sCD163)由慢性丙型肝炎病毒(HCV)感染时活化的肝巨噬细胞释放,血清水平反映肝脏疾病的严重程度。直接抗病毒药物(DAA)治疗对sCD163水平的影响以及sCD163预测肝纤维化存在的能力尚不清楚。在一项观察性与前瞻性相结合的研究中,我们旨在研究DAA治疗后sCD163的变化,探讨sCD163与组织病理学活性及纤维化之间的关联,并验证基于sCD163的纤维化评分在HCV患者中的有效性。
我们检查了三组患者:一组澳大利亚患者(n = 28)接受聚乙二醇干扰素及第一代DAA治疗,一组丹麦患者(n = 38)接受基于索磷布韦的DAA方案治疗,一组日本患者(n = 562)接受肝活检以评估肝脏活性及纤维化(采用梅塔维评分系统)。通过酶联免疫吸附测定(ELISA)对血清sCD163水平进行定量分析。
13例(46%)澳大利亚患者实现了持续病毒学应答(SVR),只有这些患者的sCD163水平显著下降(2.7(95%CI:1.9 - 3.6)mg/L 对比 4.1(2.9 - 5.7)mg/L,p = 0.008)。在丹麦组,37例(97%)患者在治疗12周后实现了SVR,sCD163水平降低了32%(5.0(4.3 - 5.8)mg/L 对比 7.4(6.3 - 8.7)mg/L,p < 0.001)。下降迅速且在停药12个月后仍持续存在(p < 0.007)。sCD163水平与炎症活性及纤维化呈平行升高(p < 0.001)。基于sCD163的纤维化评分在预测显著纤维化方面优于已有的纤维化评分(受试者操作特征曲线下面积(AUROCs):0.79(0.75 - 0.83)对比天冬氨酸转氨酶与血小板比值指数(APRI)0.73(0.69 - 0.77)、纤维化-4(FIB-4)0.7
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