联想(心理学)
膜
化学
生物物理学
芳香性
有机化学
生物化学
分子
生物
心理学
心理治疗师
作者
Aline D. de Araujo,Huy N. Hoang,Junxian Lim,Jeffrey Y. W. Mak,David P. Fairlie
标识
DOI:10.1002/anie.202203995
摘要
Aromatic groups are key mediators of protein-membrane association at cell surfaces, contributing to hydrophobic effects and π-membrane interactions. Here we show electrostatic and hydrophobic influences of aromatic ring substituents on membrane affinity and cell uptake of helical, cyclic and cell penetrating peptides. Hydrophobicity is important, but subtle changes in electrostatic surface potential, dipoles and polarizability also enhance association with phospholipid membranes and cell uptake. A combination of fluorine and sulfur substituents on an aromatic ring induces microdipoles that enhance cell uptake of 12-residue peptide inhibitors of p53-HDM2 interaction and of cell-penetrating cyclic peptides. These aromatic motifs can be readily inserted into peptide sidechains to enhance their cell uptake.
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