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将石胆酸整合到肽中用于发现肽-石胆酸杂合大环肽。

Ribosomal Incorporation of Lithocholic Acid into Peptides for the Discovery Of Peptide-Lithocholic Acid Hybrid Macrocyclic Peptides.

机构信息

State Key Laboratory of Microbial Technology, Institute of Microbial Technology, Shandong University, Qingdao 266237, China.

The MOE Key Laboratory of Spectrochemical Analysis and Instrumentation, State Key Laboratory of Physical Chemistry of Solid Surfaces, Department of Chemistry, College of Chemistry and Chemical Engineering, Xiamen University, Xiamen 361005, P.R. China.

出版信息

ACS Chem Biol. 2024 Jul 19;19(7):1440-1446. doi: 10.1021/acschembio.4c00298. Epub 2024 Jun 20.

Abstract

Peptide-bile acid hybrids offer promising drug candidates due to enhanced pharmacological properties, such as improved protease resistance and oral bioavailability. However, it remains unknown whether bile acids can be incorporated into peptide chains by the ribosome to produce a peptide-bile acid hybrid macrocyclic peptide library for target-based screening. In this study, we achieved the ribosomal incorporation of lithocholic acid (LCA)-d-tyrosine into peptide chains. This led to the construction of a peptide-LCA hybrid macrocyclic peptide library, which enabled the identification of peptides TP-2C-4L3 (targeting Trop2) and EP-2C-4L5 (targeting EphA2) with strong binding affinities. Notably, LCA was found to directly participate in binding to EphA2 and confer on the peptides improved stability and resistance to proteases. Cell staining experiments confirmed the high specificity of the peptides for targeting Trop2 and EphA2. This study highlights the benefits of LCA in peptides and paves the way for discovery of stable peptide-LCA hybrid drugs.

摘要

肽-胆酸杂合体由于增强了药理学特性,如提高了蛋白酶抗性和口服生物利用度,因此成为有前途的药物候选物。然而,目前尚不清楚核糖体是否可以将胆酸掺入肽链中,以产生用于基于靶标的筛选的肽-胆酸杂合大环肽文库。在这项研究中,我们实现了胆酸(LCA)-d-酪氨酸在肽链中的核糖体掺入。这导致了肽-LCA 杂合大环肽文库的构建,从而鉴定出与 Trop2 具有强结合亲和力的肽 TP-2C-4L3(靶向 Trop2)和与 EphA2 具有强结合亲和力的肽 EP-2C-4L5(靶向 EphA2)。值得注意的是,发现 LCA 直接参与与 EphA2 的结合,并赋予肽更好的稳定性和对蛋白酶的抗性。细胞染色实验证实了这些肽对靶向 Trop2 和 EphA2 的高特异性。本研究强调了 LCA 在肽中的益处,并为发现稳定的肽-LCA 杂合药物铺平了道路。

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