子宫内膜
信使核糖核酸
子宫
胚胎
全身给药
细胞生物学
受体
内分泌学
核糖核酸
胎盘
生物
内科学
重组DNA
化学
男科
医学
低密度脂蛋白受体
整合素
癌症研究
药理学
胚胎移植
基因表达
小干扰RNA
胚胎发生
作者
Saed Abbasi,Jairo Ortiz,Kimberly Bockley,Hongyu Feng,Emily Chen,Jordan Miller,Marina Better,C. G. Eberhart,Neomi Jerry,Justin Hanes,James Segars,Laura M. Ensign
标识
DOI:10.1038/s41565-025-02108-7
摘要
Dysfunctions of the endometrium, the uterus inner lining, can impair embryo implantation and reduce pregnancy rates. Intrauterine administration of cytokines has shown potential to improve endometrium function, but it is challenged by poor targeting and dose-limiting systemic side effects. Here we present a strategy for introducing therapeutic messenger RNA into the endometrium for the treatment of reproductive disorders. mRNA was loaded into a ligand-conjugated lipid nanoparticle (LNP), enabling multivalent interactions with the temporally overexpressed integrin receptors on the endometrial surface during the window of implantation. Conjugating the targeting ligand directly to the lipid component enhanced endometrial protein expression after intrauterine infusion and reduced systemic expression in the liver and spleen. A single infusion of granulocyte-macrophage colony-stimulating factor (GM-CSF) mRNA-loaded LNP sustained local protein expression for several hours and reduced GM-CSF systemic exposure. In a murine model of endometrial injury, GM-CSF mRNA-loaded LNP improved embryo implantation rates, outperforming recombinant GM-CSF. Our strategy demonstrates the efficacy of using mRNA to improve fertility outcomes.
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