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Medium-Chain Lipid Conjugation Facilitates Cell-Permeability and Bioactivity

化学 化学型 小分子 结合 天然产物 生物化学 细胞内 生物物理学 细胞 脂类学 脂质体 脂质双层 细胞膜 色谱法 生物 数学分析 数学 精油
作者
Johannes Morstein,Alice Capecchi,Konstantin Hinnah,ByungUk Park,Jérôme Petit-Jacques,Reid C. Van Lehn,Jean‐Louis Reymond,Dirk Trauner
出处
期刊:Journal of the American Chemical Society [American Chemical Society]
卷期号:144 (40): 18532-18544 被引量:67
标识
DOI:10.1021/jacs.2c07833
摘要

The majority of bioactive molecules act on membrane proteins or intracellular targets and therefore needs to partition into or cross biological membranes. Natural products often exhibit lipid modifications to facilitate critical molecule-membrane interactions, and in many cases their bioactivity is markedly reduced upon removal of a lipid group. However, despite its importance in nature, lipid-conjugation of small molecules is not commonly used in chemical biology and medicinal chemistry, and the effect of such conjugation has not been systematically studied. To understand the composition of lipids found in natural products, we carried out a chemoinformatic characterization of the "natural product lipidome". According to this analysis, lipidated natural products predominantly contain saturated medium-chain lipids (MCLs), which are significantly shorter than the long-chain lipids (LCLs) found in membranes and lipidated proteins. To study the usefulness of such modifications in probe design, we systematically explored the effect of lipid conjugation on five different small molecule chemotypes and find that permeability, cellular retention, subcellular localization, and bioactivity can be significantly modulated depending on the type of lipid tail used. We demonstrate that MCL conjugation can render molecules cell-permeable and modulate their bioactivity. With all explored chemotypes, MCL-conjugates consistently exhibited superior uptake or bioactivity compared to LCL-conjugates and either comparable or superior uptake or bioactivity to short-chain lipid (SCL)-conjugates. Together, our findings suggest that conjugation of small molecules with MCLs could be a powerful strategy for the design of probes and drugs.
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