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植物源新型富含赖氨酸的递送肽ERD与人S100:羧基荧光素偶联的影响、芳香族和脯氨酸残基的影响、细胞内化及穿透能力

Novel Lysine-Rich Delivery Peptides of Plant Origin ERD and Human S100: The Effect of Carboxyfluorescein Conjugation, Influence of Aromatic and Proline Residues, Cellular Internalization, and Penetration Ability.

作者信息

Sebák Fanni, Horváth Lilla Borbála, Kovács Dániel, Szolomájer János, Tóth Gábor K, Babiczky Ákos, Bősze Szilvia, Bodor Andrea

机构信息

Institute of Chemistry, ELTE-Eötvös Loránd University, Pázmány Péter sétány 1/a, H-1117 Budapest, Hungary.

Doctoral School of Pharmaceutical Sciences, Semmelweis University, Üllői út 26, H-1085 Budapest, Hungary.

出版信息

ACS Omega. 2021 Dec 6;6(50):34470-34484. doi: 10.1021/acsomega.1c04637. eCollection 2021 Dec 21.

Abstract

The need for novel drug delivery peptides is an important issue of the modern pharmaceutical research. Here, we test K-rich peptides from plant dehydrin ERD14 (ERD-A, ERD-B, and ERD-C) and the C-terminal CPP-resembling region of S100A4 (S100) using the 5(6)-carboxyfluorescein (Cf) tag at the N-terminus. Via a combined pH-dependent NMR and fluorescence study, we analyze the effect of the Cf conjugation/modification on the structural behavior, separately investigating the (5)-Cf and (6)-Cf forms. Flow cytometry results show that all peptides internalize; however, there is a slight difference between the cellular internalization of (5)- and (6)-Cf-peptides. We indicate the possible importance of residues with an aromatic sidechain and proline. We prove that ERD-A localizes mostly in the cytosol, ERD-B and S100 have partial colocalization with lysosomal staining, and ERD-C mainly localizes within vesicle-like compartments, while the uptake mechanism mainly occurs through energy-dependent paths.

摘要

新型药物递送肽的需求是现代药物研究中的一个重要问题。在此,我们使用N端带有5(6)-羧基荧光素(Cf)标签,测试了来自植物脱水素ERD14的富含赖氨酸的肽(ERD-A、ERD-B和ERD-C)以及S100A4的C端类似细胞穿透肽的区域(S100)。通过结合pH依赖性核磁共振和荧光研究,我们分析了Cf缀合/修饰对结构行为的影响,分别研究了(5)-Cf和(6)-Cf形式。流式细胞术结果表明,所有肽都能内化;然而,(5)-和(6)-Cf肽的细胞内化之间存在细微差异。我们指出了具有芳香族侧链和脯氨酸的残基的可能重要性。我们证明,ERD-A主要定位于细胞质中,ERD-B和S100与溶酶体染色有部分共定位,ERD-C主要定位于囊泡样区室中,而摄取机制主要通过能量依赖途径发生。

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