坏死性下垂
裂谷1
医学
原发性硬化性胆管炎
纤维化
程序性细胞死亡
内科学
细胞凋亡
炎症
肝损伤
胃肠病学
肝病学
肝移植
癌症研究
坏死
类有机物
炎症性肠病
胆管
渗透(HVAC)
病理
肝星状细胞
疾病
胆道
肝病
慢性肝病
效应器
胆汁淤积
英夫利昔单抗
作者
Pierre‐Antoine Soret,Virginie Steunou,Julien Hédou,Juliette Tokgozoglu,Valéria Pistorio,Amine Majdi,Nadia Darwane,J. Delaunay,Siham Benyahia,Laetitia Dinard,Tatiana Ledent,Inès Metatla,Ida Chiara Guerrera,Marie Lhomme,Maharajah Ponnaiah,Jérôme Galon,Patrick Soussan,Lawrence Serfaty,Christophe Corpechot,Chantal Housset
出处
期刊:Science Advances
[American Association for the Advancement of Science]
日期:2025-12-17
卷期号:11 (51): eadz7907-eadz7907
被引量:1
标识
DOI:10.1126/sciadv.adz7907
摘要
Primary sclerosing cholangitis (PSC) is a chronic cholestatic liver disease with no effective curative therapies. Necroptosis, a regulated necrotic cell death pathway controlled by receptor-interacting protein kinase 1 (RIPK1), has emerged as a potential driver of inflammation and fibrosis in chronic liver disorders. We investigated the role of necroptosis in PSC and whether RIPK1 inhibition could modify disease course and progression. Spatial profiling of human PSC biopsies revealed that necroptosis primarily affects cholangiocytes, while apoptosis was more frequent in hepatocytes and nonbiliary cells. In vitro, necroptosis inhibition protected cholangiocytes, and RIPK1 deletion conferred resistance to TNF-mediated cytotoxicity. In a murine model of PSC, pharmacological RIPK1 inhibition reduced cholestatic injury, hepatic inflammation, and biliary fibrosis. Multiomic analyses comprehensively demonstrated reprogramming toward wild-type–like profiles following treatment. These findings identify necroptosis as a critical effector in PSC and highlight RIPK1 inhibition as a promising disease-modifying approach, opening the door to targeted necroptosis-based therapies for this otherwise untreatable disease.
科研通智能强力驱动
Strongly Powered by AbleSci AI