Baumert Brittney O, Maretti-Mira Ana C, Li Zhenjiang, Stratakis Nikos, Zhao Yinqi, Walker Douglas I, Wang Hongxu, Fischer Fabian Christoph, Jia Qiran, Valvi Damaskini, Bartell Scott M, Chen Carmen, Inge Thomas, Ryder Justin, Jenkins Todd, Sisley Stephanie, Xanthakos Stavra, Kohli Rohit, Rock Sarah, Eckel Sandrah P, La Merrill Michele A, Aung Max M, Salomon Matthew P, McConnell Rob, Goodrich Jesse, Conti David V, Golden-Mason Lucy, Chatzi Lida
medRxiv. 2024 Jul 3:2024.07.01.24309775. doi: 10.1101/2024.07.01.24309775.
To address the growing epidemic of liver disease, particularly in pediatric populations, it is crucial to identify modifiable risk factors for the development and progression of metabolic dysfunction-associated steatotic liver disease (MASLD). Per- and polyfluoroalkyl substances (PFAS) are persistent ubiquitous chemicals and have emerged as potential risk factors for liver damage. However, their impact on the etiology and severity of MASLD remains largely unexplored in humans. This study aims to bridge the gap between human and in vitro studies to understand how exposure to perfluoroheptanoic acid (PFHpA), one of the emerging PFAS replacements which accumulates in high concentrations in the liver, contributes to MASLD risk and progression. First, we showed that PFHpA plasma concentrations were significantly associated with increased risk of MASLD in obese adolescents. Further, we examined the impact of PFHpA on hepatic metabolism using 3D human liver spheroids and single-cell transcriptomics to identify major hepatic pathways affected by PFHpA. Next, we integrated the and multi-omics datasets with a novel statistical approach which identified signatures of proteins and metabolites associated with MASLD development triggered by PFHpA exposure. In addition to characterizing the contribution of PFHpA to MASLD progression, our study provides a novel strategy to identify individuals at high risk of PFHpA-induced MASLD and develop early intervention strategies. Notably, our analysis revealed that the proteomic signature exhibited a stronger correlation between both PFHpA exposure and MASLD risk compared to the metabolomic signature. While establishing a clear connection between PFHpA exposure and MASLD progression in humans, our study delved into the molecular mechanisms through which PFHpA disrupts liver metabolism. Our findings revealed that PFHpA primarily impacts lipid metabolism, leading to a notable increase of lipid accumulation in human hepatocytes after PFHpA exposure. Among the pathways involved in lipid metabolism in hepatocytes, regulation of lipid metabolism by PPAR-a showed a remarkable activation. Moreover, the translational research framework we developed by integrating human and in vitro data provided us biomarkers to identify individuals at a high risk of MASLD due to PFHpA exposure. Our framework can inform policies on PFAS-induced liver disease and identify potential targets for prevention and treatment strategies.
为应对日益严重的肝脏疾病流行趋势,尤其是在儿科人群中,识别代谢功能障碍相关脂肪性肝病(MASLD)发生和进展的可改变风险因素至关重要。全氟和多氟烷基物质(PFAS)是普遍存在的持久性化学物质,已成为肝脏损伤的潜在风险因素。然而,它们对MASLD病因和严重程度的影响在人类中仍 largely未被探索。本研究旨在弥合人类研究和体外研究之间的差距,以了解接触全氟庚酸(PFHpA)——一种新兴的PFAS替代品,在肝脏中高浓度积累——如何导致MASLD风险和进展。首先,我们表明PFHpA血浆浓度与肥胖青少年中MASLD风险增加显著相关。此外,我们使用3D人肝球体和单细胞转录组学研究了PFHpA对肝脏代谢的影响,以确定受PFHpA影响的主要肝脏途径。接下来,我们用一种新的统计方法整合了 和 多组学数据集,该方法识别了与PFHpA暴露引发的MASLD发展相关的蛋白质和代谢物特征。除了表征PFHpA对MASLD进展的贡献外,我们的研究还提供了一种新策略,以识别PFHpA诱导的MASLD高风险个体并制定早期干预策略。值得注意的是,我们的分析表明,与代谢组学特征相比,蛋白质组学特征在PFHpA暴露和MASLD风险之间表现出更强的相关性。在建立PFHpA暴露与人类MASLD进展之间的明确联系时,我们的研究深入探讨了PFHpA破坏肝脏代谢的分子机制。我们的 研究结果表明,PFHpA主要影响脂质代谢,导致PFHpA暴露后人类肝细胞中脂质积累显著增加。在肝细胞脂质代谢涉及的途径中,PPAR-α对脂质代谢的调节显示出显著激活。此外,我们通过整合人类和体外数据开发的转化研究框架为我们提供了生物标志物,以识别因PFHpA暴露而患MASLD高风险的个体。我们的框架可为PFAS诱导的肝病政策提供信息,并确定预防和治疗策略的潜在靶点。 (注:原文中“ 和 ”部分内容缺失,翻译时保留原样)
