化学
向性
信使核糖核酸
肺
内皮
细胞生物学
运输机
内皮干细胞
体外
体内
血管舒张
肺动脉高压
药理学
内体
血管
阳离子聚合
肝素
生物化学
细胞内
细胞
HEK 293细胞
组织向性
生物物理学
作者
Mahmoud M. AbdElwakil,Jeffrey Ni,Summer Ramsay-Burrough,Paul J. Hurst,Rebecca L. McClellan,Samuel R. Khasnavis,Yuan Jia,Salwa Masud,Timothy R. Blake,Adrienne Sallets,Ole Audun Werner Haabeth,Idit Sagiv-Barfi,Debra K. Czerwinski,Marco Herrera‐Barrera,Ronald Levy,Paul A. Wender,Maya E. Kumar,Robert M. Waymouth
摘要
Endothelial cells (ECs) comprise the pulmonary vascular bed and play a significant role in health and diseases. Consequently, the EC niche represents an attractive therapeutic target for treating a wide range of pulmonary vascular diseases. We have identified a new class of dicationic charge-altering releasable transporters. These single-component transporters selectively deliver mRNA to the lung upon intravenous administration without the use of a targeting ligand. Significantly, the number and spatial array of cationic charges within the repeating units of the CART polymer are found to control both mRNA delivery efficacy and tissue tropism. High-resolution imaging revealed efficient mRNA delivery to endothelial cells in pulmonary arteries, veins, and capillaries. The selective lung tropism of these new CARTs, coupled with the efficient and tunable synthesis of this new family of CART amphiphiles, represents an enabling platform for research and clinical applications.
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