细胞毒性T细胞
重编程
体内
效应器
CD8型
细胞生物学
化学
离体
白细胞介素21
体外
生物
白细胞介素2受体
自然杀伤性T细胞
抗原提呈细胞
免疫学
T细胞
分子生物学
ZAP70型
CD28
白细胞介素12
脾脏
免疫系统
CTL公司*
癌症研究
作者
Angela R. Corrigan,Shin Foong Ngiow,Maura Statzu,M. Betina Pampena,Jayme M.L. Nordin,Amie Albertus,Stephen D. Carro,Justin Harper,Rachelle L. Stammen,Jennifer Wood,Jacob T. Hamilton,Houping Ni,Justin Su,Rajesvaran Ramalingam,Vincent H. Wu,Mirko Paiardini,Drew Weissman,E. John Wherry,Edward F. Kreider,Michael R. Betts
出处
期刊:
[Cold Spring Harbor Laboratory]
日期:2025-10-30
被引量:1
标识
DOI:10.1101/2025.10.29.685358
摘要
Abstract Selective in vivo reprogramming of cytotoxic effector CD8 + T (T eff ) cells holds tremendous promise as a therapeutic tool but has not yet been accomplished. Here, we demonstrate that fractalkine-conjugated mRNA lipid nanoparticles (mRNA-LNP) can specifically target and deliver mRNA to CX3CR1 + T eff cells in vitro and in vivo. In mice, fractalkine-conjugated LNP target up to 90% of blood and splenic T eff cells, and delivery of IL-2-encoding mRNA to T eff cells enables robust exogenous IL-2 secretion. In rhesus macaques, fractalkine-conjugated mRNA-LNP target up to ∼100% of peripheral blood T eff cells and delivery of CD62L-mRNA enables transient CD62L expression. Collectively, these data demonstrate the potential of natural receptor ligand-based targeting of mRNA-LNP for effective and efficient transient in vivo modification of T eff cells.
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