Authors
Zilu Li, Jie Qin, Jiayu Zhang, Yumiao Chen, Daohan Yu, Yiran Zhang, Shengfei Yang, Zhuoting Li, Juanjuan Zheng, Jinquan Cai, Fan Huang, Jianqing Gao, Yu Zhao
Published in
Science advances. Volume 12. Issue 27. Pages eaef1695. Jul 03, 2026. Epub Jul 01, 2026.
Abstract
Lipid nanoparticles (LNPs), composed of ionizable lipids, phospholipids, cholesterol, and PEGylated lipids, have been successfully used in messenger RNA (mRNA) vaccine development. Despite substantial progress, endosomal entrapment after cellular internalization is still a critical bottleneck limiting the vaccine efficacy. While the efforts to optimize lipid pKa, spatial conformation, and LNP composition have been made, further fine-tuning of these parameters shows diminishing returns in improving effectiveness. Here, we propose a previously unreported parameter, programmable mechanical movement. LNPs are expected to destabilize endosomal membranes through conducting mechanical movements under specific inputs, achieving robust endosomal escape. Specifically, we demonstrate a light-emitting diode (LED)-driven movable lipid (i.e., phenylazothiazole lipid) capable of performing mechanical movements. We integrate the movable lipids into the BNT162b2 formulation from Pfizer-BioNTech. Upon LED irradiation, the movable lipids within LNPs function as molecular rotors, thereby facilitating endosomal membrane destabilization. This strategy has achieved exciting preclinical results in enhancing mRNA-LNP cancer vaccine efficacy.
PMID:
42384808
Bibliographic data and abstract were imported from PubMed on 02 Jul 2026.
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