血浆组织蛋白酶D作为酒精性肝病的早期指标。
Plasma cathepsin D as an early indicator of alcohol-related liver disease.
作者信息
Li Mengying, Houben Tom, Bitorina Albert V, Meesters Dennis M, Israelsen Mads, Kjærgaard Maria, Koek Ger H, Hendrikx Tim, Verbeek Jef, Krag Aleksander, Thiele Maja, Shiri-Sverdlov Ronit
机构信息
Department of Genetics and Cell Biology, Institute of Nutrition and Translational Research in Metabolism, Maastricht University, the Netherlands.
Center for Liver Research, Odense University Hospital and University of Southern Denmark, Kloevervaenget 10, entrance 112, DK-5000 Odense, Denmark.
出版信息
JHEP Rep. 2024 May 9;6(9):101117. doi: 10.1016/j.jhepr.2024.101117. eCollection 2024 Sep.
BACKGROUND & AIMS: People who drink alcohol excessively are at increased risk of developing metabolic dysfunction and alcohol-related liver disease (MetALD) or the more severe form alcohol-related liver disease (ALD). One of the most significant challenges concerns the early detection of MetALD/ALD. Previously, we have demonstrated that the lysosomal enzyme cathepsin D (CTSD) is an early marker for metabolic dysfunction-associated steatohepatitis (MASH). Here, we hypothesized that plasma CTSD can also serve as an early indicator of MetALD/ALD.
METHODS
We included 303 persistent heavy drinkers classified as having MetALD or ALD (n = 152) and abstinent patients with a history of excessive drinking (n = 151). Plasma CTSD levels of patients with MetALD/ALD without decompensation were compared with 40 healthy controls. Subsequently, the relationship between plasma CTSD levels and hepatic histological scores was established. Receiver-operating characteristic curves were generated to assess the precision of plasma CTSD levels in detecting MetALD/ALD. Lastly, plasma CTSD levels were compared between abstainers and drinkers.
RESULTS
Plasma CTSD levels were higher in patients with MetALD/ALD compared to healthy controls. While hepatic disease parameters (AST/ALT ratio, liver stiffness measurement) were higher at advanced histopathological stages (assessed by liver biopsy), plasma CTSD levels were already elevated at early histopathological stages. Furthermore, combining plasma CTSD levels with liver stiffness measurement and AST/ALT ratio yielded enhanced diagnostic precision (AUC 0.872) in detecting MetALD/ALD in contrast to the utilization of CTSD alone (AUC 0.804). Plasma CTSD levels remained elevated in abstainers.
CONCLUSION
Elevated levels of CTSD in the circulation can serve as an early indicator of MetALD/ALD.
IMPACT AND IMPLICATIONS
Alcohol-related liver disease is the leading cause of liver disease-related morbidity and mortality worldwide. However, the currently available non-invasive methods to diagnose MetALD/ALD are only able to detect advanced stages of MetALD/ALD. Here, we demonstrate that plasma levels of the lysosomal enzyme cathepsin D are already elevated at early stages of MetALD/ALD. Moreover, cathepsin D levels outperformed the currently available non-invasive methods to detect MetALD/ALD. Plasma levels of cathepsin D could therefore be a useful non-invasive marker for detection of MetALD/ALD.
背景与目的
过度饮酒者发生代谢功能障碍以及酒精性肝病(MetALD)或更严重形式的酒精性肝病(ALD)的风险增加。其中最重大的挑战之一是MetALD/ALD的早期检测。此前,我们已证明溶酶体酶组织蛋白酶D(CTSD)是代谢功能障碍相关脂肪性肝炎(MASH)的早期标志物。在此,我们假设血浆CTSD也可作为MetALD/ALD的早期指标。
方法
我们纳入了303名持续性重度饮酒者,其中被归类为患有MetALD或ALD的有152人,有过度饮酒史的戒酒者有151人。将无失代偿的MetALD/ALD患者的血浆CTSD水平与40名健康对照者进行比较。随后,确定血浆CTSD水平与肝脏组织学评分之间的关系。生成受试者操作特征曲线以评估血浆CTSD水平检测MetALD/ALD的准确性。最后,比较戒酒者和饮酒者的血浆CTSD水平。
结果
与健康对照者相比,MetALD/ALD患者的血浆CTSD水平更高。虽然在组织病理学晚期阶段(通过肝活检评估)肝病参数(AST/ALT比值、肝脏硬度测量)更高,但血浆CTSD水平在组织病理学早期阶段就已升高。此外,与单独使用CTSD相比,将血浆CTSD水平与肝脏硬度测量和AST/ALT比值相结合在检测MetALD/ALD时具有更高的诊断准确性(曲线下面积为0.872)。戒酒者的血浆CTSD水平仍升高。
结论
循环中CTSD水平升高可作为MetALD/ALD的早期指标。
影响与意义
酒精性肝病是全球范围内肝病相关发病率和死亡率的主要原因。然而,目前可用的诊断MetALD/ALD的非侵入性方法仅能检测到MetALD/ALD的晚期阶段。在此,我们证明在MetALD/ALD的早期阶段,溶酶体酶组织蛋白酶D的血浆水平就已升高。此外,组织蛋白酶D水平优于目前可用的检测MetALD/ALD的非侵入性方法。因此,组织蛋白酶D的血浆水平可能是检测MetALD/ALD的有用非侵入性标志物。
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