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Synthesis and Purification of Homogeneous Lipid-BasedPeptide Nanocarriers by Overcoming Phospholipid Ester Hydrolysis

机译:均相脂质基的合成与纯化克服磷脂酯水解作用的肽纳米载体

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摘要

Despite the therapeutic promise of phospholipid-based nanocarriers, a major obstacle to their widespread clinical translation is a susceptibility to fatty acid ester hydrolysis, leading to lack of quality control and inconsistencies in self-assembly formulations. Using electrospray ionization mass spectrometry fragmentation in combination with matrix-assisted laser desorption/ionization time-of-flight mass spectrometry, we have demonstrated a method to detect hydrolysis of one or both of the fatty acid esters in a PEGylated phospholipid, DSPE-PEG, in conditions commonly applied during nanocarrier production. Because such carriers are increasingly being used to deliver peptide-based therapeutics, we further investigated the hydrolysis of phospholipid esters in conditions used for solid-phase peptide synthesis and high-performance liquid chromatography of peptides. We ultimately detail a synthetic strategy to reliably produce pure phospholipid–peptide bioconjugates (peptide amphiphiles), while avoiding unintended or unnoticed hydrolyzed byproducts that could lead to polymorphic nanotherapeutics with dampened therapeutic efficacy.We believe that such an approach could help standardize phospholipid–peptide-basedtherapeutic development, testing, and clinical translation.
机译:尽管基于磷脂的纳米载体具有治疗前景,但其广泛的临床翻译的主要障碍是脂肪酸酯水解的敏感性,导致缺乏质量控制和自组装制剂的不一致。结合电喷雾电离质谱碎片化技术和基质辅助激光解吸/电离飞行时间质谱技术,我们证明了一种检测PEG化磷脂DSPE-PEG中一种或两种脂肪酸酯水解的方法,在纳米载体生产过程中通常使用的条件下。由于此类载体越来越多地用于提供基于肽的治疗剂,因此我们在固相肽合成和肽的高效液相色谱所用的条件下进一步研究了磷脂酯的水解。我们最终详细描述了一种可靠地生产纯磷脂-肽生物共轭物(肽两亲物)的合成策略,同时避免了可能会导致多态性纳米疗法治疗效果减弱的意外或未引起注意的水解副产物。我们认为,这种方法可以帮助标准化基于磷脂-肽的治疗性开发,测试和临床翻译。

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