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源自 Serpin A1 的反向胶原调制肽,具有增强的稳定性和体外活性。

Retro-Inverso Collagen Modulator Peptide Derived from Serpin A1 with Enhanced Stability and Activity In Vitro.

机构信息

Department of Neurosciences, Psychology, Drug Research and Child Health, University of Florence, Sesto Fiorentino, FI 50019, Italy.

Interdepartmental Laboratory of Peptide and Protein Chemistry and Biology, University of Florence, Sesto Fiorentino, FI 50019, Italy.

出版信息

J Med Chem. 2024 Mar 28;67(6):5053-5063. doi: 10.1021/acs.jmedchem.4c00137. Epub 2024 Mar 12.

Abstract

The rising demand for novel cosmeceutical ingredients has highlighted peptides as a significant category. Based on the collagen turnover modulation properties of SA1-III, a decapeptide derived from a serine protease inhibitor (serpin A1), this study focused on designing shorter, second-generation peptides endowed with improved properties. A tetrapeptide candidate was further modified employing the retro-inverso approach that uses d-amino acids aiming to enhance peptide stability against dermal enzymes. Surprisingly, the modified peptide AAT11RI displayed notably high activity in vitro, as compared to its precursors, and suggested a mode of action based on the inhibition of collagen degradation. It is worth noting that AAT11RI showcases stability against dermal enzymes contained in human skin homogenates due to its rationally designed structure that hampers recognition by most proteases. The rational approach we embraced in this study underscored the added value of substantiated claims in the design of new cosmeceutical ingredients, representing a rarity in the field.

摘要

新型化妆品成分的需求不断增长,凸显出肽类物质的重要性。本研究基于来源于丝氨酸蛋白酶抑制剂(serpin A1)的十肽 SA1-III 对胶原蛋白周转率的调节特性,专注于设计具有改良性能的更短第二代肽。进一步采用反向肽策略修饰一个四肽候选物,该策略使用 d-氨基酸旨在增强肽对皮肤酶的稳定性。令人惊讶的是,与前体相比,经修饰的肽 AAT11RI 在体外表现出显著的高活性,并提出了一种基于抑制胶原蛋白降解的作用模式。值得注意的是,由于其合理设计的结构阻止了大多数蛋白酶的识别,因此 AAT11RI 展示了对包含在人体皮肤匀浆中的皮肤酶的稳定性。我们在这项研究中采用的合理方法强调了在设计新型化妆品成分时,有充分依据的主张的附加值,这在该领域是罕见的。

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