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首页> 外文期刊>Biochimica et biophysica acta. Bioenergetics >Membrane adsorption and binding, cellular uptake and cytotoxicity of cell-penetrating peptidomimetics with α-peptide/β-peptoid backbone: effects of hydrogen bonding and α-chirality in the β-peptoid residues.
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Membrane adsorption and binding, cellular uptake and cytotoxicity of cell-penetrating peptidomimetics with α-peptide/β-peptoid backbone: effects of hydrogen bonding and α-chirality in the β-peptoid residues.

机译:具有α-肽/β-类肽骨架的细胞穿透拟肽的膜吸附和结合,细胞摄取和细胞毒性:β-类肽残基中氢键和α-手性的影响。

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摘要

Cell-penetrating peptides (CPPs) provide a promising approach for enhancing intracellular delivery of therapeutic biomacromolecules by increasing transport through membrane barriers. Here, proteolytically stable cell-penetrating peptidomimetics with α-peptide/β-peptoid backbone were studied to evaluate the effect of α-chirality in the β-peptoid residues and the presence of guanidinium groups in the α-amino acid residues on membrane interaction. The molecular properties of the peptidomimetics in solution (surface and intramolecular hydrogen bonding, aqueous diffusion rate and molecular size) were studied along with their adsorption to lipid bilayers, cellular uptake, and toxicity. The surface hydrogen bonding ability of the peptidomimetics reflected their adsorbed amounts onto lipid bilayers as well as with their cellular uptake, indicating the importance of hydrogen bonding for their membrane interaction and cellular uptake. Ellipsometry studies further demonstrated that the presence of chiral centers in the β-peptoid residues promotes a higher adsorption to anionic lipid bilayers, whereas circular dichroism results showed that α-chirality influences their overall mean residue ellipticity. The presence of guanidinium groups and α-chiral β-peptoid residues was also found to have a significant positive effect on uptake in living cells. Together, the findings provide an improved understanding on the behavior of cell-penetrating peptidomimetics in the presence of lipid bilayers and live cells.
机译:细胞穿透肽(CPPs)提供了一种有前途的方法,可通过增加通过膜屏障的转运来增强治疗性生物大分子的细胞内递送。在此,研究了具有α-肽/β-类肽骨架的蛋白水解稳定的细胞渗透拟肽,以评估β-类肽残基中的α-手性和α-氨基酸残基中胍基的存在对膜相互作用的影响。研究了拟肽在溶液中的分子性质(表面和分子内氢键,水扩散速率和分子大小),以及它们对脂质双层的吸附,细胞摄取和毒性。拟肽的表面氢键结合能力反映了它们在脂质双层上的吸附量以及它们的细胞吸收,表明氢键对于它们的膜相互作用和细胞吸收很重要。椭偏分析进一步证明,β-类肽残基中存在手性中心可促进对阴离子脂质双层的更高吸附,而圆二色性结果表明,α-手性会影响其总体平均残基椭圆率。还发现胍基和α-手性β-类肽残基的存在对活细胞的摄取具有显着的积极影响。在一起,这些发现提供了在脂质双层和活细胞存在下细胞穿透拟肽的行为的更好的理解。

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