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利用同型精氨酸获得衰减的阳离子膜溶肽。

Use of homoarginine to obtain attenuated cationic membrane lytic peptides.

机构信息

Institute for Chemical Research, Kyoto University, Uji, Kyoto 611-0011, Japan.

Institute for Chemical Research, Kyoto University, Uji, Kyoto 611-0011, Japan.

出版信息

Bioorg Med Chem Lett. 2021 May 15;40:127925. doi: 10.1016/j.bmcl.2021.127925. Epub 2021 Mar 9.

Abstract

Our research group has been studying the design of intracellular delivery peptides based on cationic lytic peptides. By placing negatively charged amino acids on potentially hydrophobic faces of the peptides, membrane lytic activity is attenuated on the cell surface, whereas it recovers in endosomes, enabling cytosolic delivery of proteins including antibodies. These lytic peptides generally contain multiple lysines, facilitating cell surface interaction and membrane perturbation. This study evaluated the effect of lysine-to-homoarginine substitution using HAad as a model delivery peptide. The resulting peptide had a comparable or better delivery efficacy for Cre recombinase, antibodies, and the Cas9/sgRNA complex with one-quarter of the concentration of HAad, implying that a subtle structural difference can affect delivery activity.

摘要

我们的研究小组一直在研究基于阳离子裂解肽的细胞内递药肽的设计。通过在肽的潜在疏水面上放置带负电荷的氨基酸,可以在细胞表面上减弱膜裂解活性,而在内体中恢复,从而实现包括抗体在内的蛋白质的细胞质递药。这些裂解肽通常含有多个赖氨酸,有利于细胞表面相互作用和膜扰动。本研究使用 HAad 作为模型递药肽来评估赖氨酸到同型精氨酸取代的效果。所得肽对 Cre 重组酶、抗体和 Cas9/sgRNA 复合物的递药效果相当或更好,其浓度为 HAad 的四分之一,这表明细微的结构差异会影响递药活性。

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