α1抗胰蛋白酶聚合物负荷与肝细胞衰老、纤维化阶段及肝脏相关死亡率相关。
The Alpha-1 Antitrypsin Polymer Load Correlates With Hepatocyte Senescence, Fibrosis Stage and Liver-Related Mortality.
作者信息
Mela Marianna, Smeeton Wendy, Davies Susan E, Miranda Elena, Scarpini Cinzia, Coleman Nick, Alexander Graeme J M
机构信息
Division of Gastroenterology and Hepatology, University Department of Medicine, Addenbrooke's Hospital, Cambridge, United Kingdom.
Department of Histopathology, Addenbrooke's Hospital, Cambridge, United Kingdom.
出版信息
Chronic Obstr Pulm Dis. 2020 Jul;7(3):151-162. doi: 10.15326/jcopdf.7.3.2019.0158.
BACKGROUND
Alpha-1 antitrypsin deficiency (AATD) is an important, inherited cause of chronic liver disease. Marked variation in fibrosis stages in patients with homozygous deficiency and those factors that determine whether heterozygous carriers develop liver fibrosis, remain unexplained. Murine studies implicate polymerized alpha-1 antitrypsin (AAT) within hepatocytes as pathogenic.
AIMS AND METHODS
The relationship between the quantity of polymerized AAT within hepatocytes (polymer load), stage of hepatic fibrosis and liver-related clinical outcomes (death, evolution to hepatocellular carcinoma, or need for liver transplantation) were investigated using liver tissue from 92 patients at first presentation with either homozygous or heterozygous AATD. Further tissue-based studies were undertaken to determine if polymerized AAT was associated with failure of cell cycle progression, accelerated aging or hepatocyte senescence by immunohistochemical analysis.
RESULTS
The AAT polymer load correlated closely with hepatic fibrosis stage and long-term clinical outcome, independent of homozygous or heterozygous status. AAT polymers within hepatocytes correlated closely with failure of cell cycle progression assessed using cell cycle phase markers, accelerated aging manifest as shortened telomeres and other markers consistent with hepatocyte senescence manifest as the presence of nuclear p21 expression and enlarged nuclei. The proportion of p21 positive hepatocytes or hepatocytes with enlarged nuclei correlated with hepatic fibrosis stage and the long-term clinical outcome.
CONCLUSION
These data suggest that accumulation of AAT polymers within hepatocytes drives senescence. Quantitation of both the AAT polymer load or hepatocyte senescence markers correlated with hepatic fibrosis stage and the long-term clinical outcome. Either or both could be considered markers of disease severity and treatment response in clinical trials.
背景
α-1抗胰蛋白酶缺乏症(AATD)是慢性肝病的一个重要遗传性病因。纯合子缺乏患者纤维化阶段的显著差异以及决定杂合子携带者是否发生肝纤维化的因素仍不清楚。小鼠研究表明肝细胞内聚合的α-1抗胰蛋白酶(AAT)具有致病性。
目的和方法
使用92例首次就诊的纯合子或杂合子AATD患者的肝组织,研究肝细胞内聚合AAT的量(聚合物负荷)、肝纤维化阶段与肝脏相关临床结局(死亡、进展为肝细胞癌或需要肝移植)之间的关系。通过免疫组织化学分析进行进一步的基于组织的研究,以确定聚合AAT是否与细胞周期进程失败、加速衰老或肝细胞衰老有关。
结果
AAT聚合物负荷与肝纤维化阶段和长期临床结局密切相关,与纯合子或杂合子状态无关。肝细胞内的AAT聚合物与使用细胞周期阶段标志物评估的细胞周期进程失败密切相关,加速衰老表现为端粒缩短,其他与肝细胞衰老一致的标志物表现为核p21表达和细胞核增大。p21阳性肝细胞或细胞核增大的肝细胞比例与肝纤维化阶段和长期临床结局相关。
结论
这些数据表明肝细胞内AAT聚合物的积累驱动衰老。AAT聚合物负荷或肝细胞衰老标志物的定量与肝纤维化阶段和长期临床结局相关。在临床试验中,两者之一或两者都可被视为疾病严重程度和治疗反应的标志物。
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