Patient-derived liver organoids recapitulate liver epithelial heterogeneity and enable precision modeling of alcohol-related liver disease.

IF 33 1区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY

Journal of Hepatology Pub Date : 2025-08-01 DOI:10.1016/j.jhep.2025.07.014

Silvia Ariño, Raquel Ferrer-Lorente, Guillermo Serrano, Laura Zanatto, Raquel A Martínez-García de la Torre, Jordi Gratacós-Ginès, Ana Belén Rubio, Martina Pérez, Carlos Mateos-Sánchez, Beatriz Aguilar-Bravo, Stephen Atkinson, Zhengqing Xu, Paula Cantallops-Vilà, Laura Sererols-Viñas, Paloma Ruiz-Blázquez, Aina Rill, Yiliam Fundora, Juan José Lozano, Mar Coll, Idoia Ochoa, Silvia Affo, Anna Moles, Elisabetta Mereu, Ramón Bataller, Elisa Pose, Pau Sancho-Bru

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引用次数: 0

Abstract

Background & aims: Alcohol-associated liver disease (ALD) is a major cause of liver disease worldwide with scarce therapeutic options. Animal models poorly recapitulate advanced ALD precluding the development of new treatments. Organoids have emerged as a powerful human-based preclinical tool. However, current patient-derived liver organoids fail to recapitulate the epithelial heterogeneity and its generation requires liver surgical resections, thus limiting personalized disease modeling. Here, we report the development of organoids from liver needle biopsies (b-Orgs) from patients with ALD.

Methods: b-Orgs were generated from tru-cut biopsies from patients at early (n=28) and advanced (n=34) stages of ALD. b-Orgs were characterized by immunofluorescence, bulk and single cell RNA-sequencing and compared to parental tissues. b-Orgs were used to model ALD progression, identify pathogenic drivers, induce alcohol-associated hepatitis (AH) and evaluate response to prednisolone.

Results: Phenotypic and functional analysis of b-Orgs showed hepatocyte-enriched features. Single-cell RNA-sequencing revealed a heterogeneous cell composition comprising hepatocyte, biliary and progenitor populations, mirroring the epithelial landscape found in patients with advanced ALD. Moreover, b-Orgs preserved disease-stage features and allowed to identify the association of ELF3 with cell plasticity and disease progression. Finally, stimulation of b-Orgs with drivers of ALD induced pathophysiological features of alcohol-associated hepatitis, including ROS production, lipid accumulation, inflammation and decreased cell proliferation, which were mitigated in response to prednisolone.

Conclusions: Overall, we provide a human-based model that captures the epithelial complexity and specific patient features. This approach helps to identify drivers of cell plasticity and expanding organoid-based liver disease modeling for personalized medicine.

Impact and implications: Here, we describe the generation of biopsy-derived organoids (b-Orgs) from patients with liver disease. b-Orgs capture the liver epithelial cell composition found in patients' liver tissue and are efficiently generated from different stages of the disease, providing a platform for patient-tailored disease modeling and drug testing.

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患者来源的肝类器官概括了肝上皮的异质性，并使酒精相关肝病的精确建模成为可能。

背景与目的：酒精相关性肝病（ALD）是世界范围内肝脏疾病的主要原因，治疗方案很少。动物模型不能很好地概括晚期ALD，阻碍了新治疗方法的发展。类器官已经成为一种强大的基于人类的临床前工具。然而，目前患者来源的肝类器官不能再现上皮异质性，其生成需要肝脏手术切除，因此限制了个性化疾病建模。在这里，我们报告了ALD患者肝穿刺活检（b-Orgs）中类器官的发展。方法：从早期（n=28）和晚期（n=34） ALD患者的真切活检中产生b组织。通过免疫荧光、整体和单细胞rna测序对b-Orgs进行了表征，并与亲代组织进行了比较。b-Orgs用于模拟ALD进展，确定致病因素，诱导酒精相关性肝炎（AH）并评估对泼尼松龙的反应。结果：b-Orgs的表型和功能分析显示肝细胞富集。单细胞rna测序揭示了由肝细胞、胆道细胞和祖细胞组成的异质性细胞组成，反映了晚期ALD患者的上皮景观。此外，b-Orgs保留了疾病分期特征，并允许鉴定ELF3与细胞可塑性和疾病进展的关联。最后，通过ALD驱动刺激b-Orgs诱导酒精相关性肝炎的病理生理特征，包括ROS生成、脂质积累、炎症和细胞增殖下降，这些在泼尼松龙的作用下得到缓解。结论：总的来说，我们提供了一个基于人类的模型，可以捕捉上皮复杂性和特定的患者特征。这种方法有助于识别细胞可塑性的驱动因素，并扩大基于类器官的肝病建模，用于个性化医疗。影响和意义：在这里，我们描述了肝脏疾病患者活检来源的类器官（b-Orgs）的产生。b-Orgs捕获患者肝组织中发现的肝上皮细胞组成，并在疾病的不同阶段有效地产生，为患者量身定制的疾病建模和药物测试提供了平台。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Hepatology 医学-胃肠肝病学

CiteScore

46.10

自引率

4.30%

发文量

2325

审稿时长

30 days

期刊介绍： The Journal of Hepatology is the official publication of the European Association for the Study of the Liver (EASL). It is dedicated to presenting clinical and basic research in the field of hepatology through original papers, reviews, case reports, and letters to the Editor. The Journal is published in English and may consider supplements that pass an editorial review.