Department of Medicine, Section of Gastroenterology, Center for Regenerative Medicine, Boston University Chobanian & Avedisian School of Medicine & Boston Medical Center, Boston, MA, USA.
Acuitas Therapeutics, Vancouver, BC, Canada.
Nat Commun. 2024 Jun 12;15(1):5010. doi: 10.1038/s41467-024-49332-8.
Primary human hepatocyte (PHH) transplantation is a promising alternative to liver transplantation, whereby liver function could be restored by partial repopulation of the diseased organ with healthy cells. However, currently PHH engraftment efficiency is low and benefits are not maintained long-term. Here we refine two male mouse models of human chronic and acute liver diseases to recapitulate compromised hepatocyte proliferation observed in nearly all human liver diseases by overexpression of p21 in hepatocytes. In these clinically relevant contexts, we demonstrate that transient, yet robust expression of human hepatocyte growth factor and epidermal growth factor in the liver via nucleoside-modified mRNA in lipid nanoparticles, whose safety was validated with mRNA-based COVID-19 vaccines, drastically improves PHH engraftment, reduces disease burden, and improves overall liver function. This strategy may overcome the critical barriers to clinical translation of cell therapies with primary or stem cell-derived hepatocytes for the treatment of liver diseases.
原发性人肝细胞 (PHH) 移植是肝移植的一种有前途的替代方法,通过用健康细胞部分再殖病变器官可以恢复肝功能。然而,目前 PHH 植入效率低,且益处不能长期维持。在这里,我们改进了两种男性小鼠模型的人类慢性和急性肝病,以重现几乎所有人类肝病中观察到的受损肝细胞增殖,方法是在肝细胞中过表达 p21。在这些临床相关的情况下,我们通过核苷修饰的 mRNA 在脂质纳米粒中证明了人肝细胞生长因子和表皮生长因子在肝脏中的短暂但强大的表达,其安全性已通过基于 mRNA 的 COVID-19 疫苗得到验证,大大提高了 PHH 的植入效率,降低了疾病负担,并改善了整体肝功能。该策略可能克服了将原发性或干细胞来源的肝细胞用于治疗肝脏疾病的细胞疗法的临床转化的关键障碍。
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