Wang Feng, Hui Simon T, Stappenbeck Frank, Kaminska Dorota, Lusis Aldons J, Parhami Farhad
MAX BioPharma Inc., Santa Monica, CA 90404, USA.
Department of Medicine, Division of Cardiology, David Geffen School of Medicine, University of California, Los Angeles, CA 90095, USA.
Cells. 2025 Aug 2;14(15):1191. doi: 10.3390/cells14151191.
Senescence, a state of permanent cell cycle arrest, is a complex cellular phenomenon closely affiliated with age-related diseases and pathological fibrosis. Cellular senescence is now recognized as a significant contributor to organ fibrosis, largely driven by transforming growth factor beta (TGF-β) signaling, such as in metabolic dysfunction-associated steatohepatitis (MASH), idiopathic pulmonary fibrosis (IPF), chronic kidney disease (CKD), and myocardial fibrosis, which can lead to heart failure, cystic fibrosis, and fibrosis in pancreatic tumors, to name a few. MASH is a progressive inflammatory and fibrotic liver condition that has reached pandemic proportions, now considered the largest non-viral contributor to the need for liver transplantation.
We previously studied Oxy210, an anti-fibrotic and anti-inflammatory, orally bioavailable, oxysterol-based drug candidate for MASH, using APOE*3-Leiden.CETP mice, a humanized hyperlipidemic mouse model that closely recapitulates the hallmarks of human MASH. In this model, treatment of mice with Oxy210 for 16 weeks caused significant amelioration of the disease, evidenced by reduced hepatic inflammation, lipid deposition, and fibrosis, atherosclerosis and adipose tissue inflammation.
Here we demonstrate increased hepatic expression of senescence-associated genes and senescence-associated secretory phenotype (SASP), correlated with the expression of pro-fibrotic and pro-inflammatorygenes in these mice during the development of MASH that are significantly inhibited by Oxy210. Using the HepG2 human hepatocyte cell line, we demonstrate the induced expression of senescent-associated genes and SASP by TGF-β and inhibition by Oxy210.
These findings further support the potential therapeutic effects of Oxy210 mediated in part through inhibition of senescence-driven hepatic fibrosis and inflammation in MASH and perhaps in other senescence-associated fibrotic diseases.
衰老,即细胞周期永久停滞的状态,是一种与年龄相关疾病及病理性纤维化密切相关的复杂细胞现象。细胞衰老目前被认为是器官纤维化的一个重要促成因素,主要由转化生长因子β(TGF-β)信号传导驱动,比如在代谢功能障碍相关脂肪性肝炎(MASH)、特发性肺纤维化(IPF)、慢性肾脏病(CKD)以及心肌纤维化中,这些情况可导致心力衰竭、囊性纤维化以及胰腺肿瘤纤维化等诸多病症。MASH是一种进展性炎症性和纤维化性肝病,已达到流行程度,目前被认为是肝移植需求的最大非病毒促成因素。
我们之前使用APOE*3-莱顿.CETP小鼠(一种高度模拟人类MASH特征的人源化高脂血症小鼠模型)研究了Oxy210,这是一种用于治疗MASH的抗纤维化、抗炎、口服生物可利用的基于氧化甾醇的候选药物。在该模型中,用Oxy210治疗小鼠16周可显著改善疾病,表现为肝脏炎症、脂质沉积和纤维化、动脉粥样硬化以及脂肪组织炎症减轻。
在此我们证明,在MASH发展过程中,衰老相关基因和衰老相关分泌表型(SASP)在这些小鼠肝脏中的表达增加,这与促纤维化和促炎基因的表达相关,而Oxy210可显著抑制这些表达。使用HepG2人肝细胞系,我们证明了TGF-β可诱导衰老相关基因和SASP的表达,而Oxy210可抑制这种表达。
这些发现进一步支持了Oxy210的潜在治疗作用,其部分作用机制可能是通过抑制MASH中衰老驱动的肝纤维化和炎症,或许在其他与衰老相关的纤维化疾病中也有作用。
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