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肽的时空自组装决定了癌症选择性毒性。

Spatiotemporal Self-Assembly of Peptides Dictates Cancer-Selective Toxicity.

机构信息

Department of Chemistry, School of Natural Science, Ulsan National Institute of Science and Technology (UNIST), Ulsan 44919, Republic of Korea.

School of Materials Science and Engineering, Gwangju Institute of Science and Technology (GIST), Gwangju 61005, Republic of Korea.

出版信息

Biomacromolecules. 2020 Dec 14;21(12):4806-4813. doi: 10.1021/acs.biomac.0c01000. Epub 2020 Sep 11.

Abstract

The intracellular or pericellular self-assembly of amphiphilic peptides is emerging as a potent cancer therapeutic strategy. Achieving the self-assembly of amphiphilic peptides inside a cell or cellular organelle is challenging due to the complex cellular environment, which consists of many amphiphilic biomolecules that may alter the self-assembling propensity of the synthetic peptides. Herein, we show that the hydrophobic-hydrophilic balance of the amphiphilic peptides determines the self-assembling propensity, thereby controlling the fate of the cell. A series of peptides were designed to target and self-assemble inside the mitochondria of cancer cells. The hydrophobicity of the peptides was tuned by varying their N-terminus capping. The analysis showed that the largest hydrophobic peptide was self-assembled before reaching the mitochondria and showed no selectivity toward cancer cells, whereas hydrophilic peptides could not self-assemble inside the mitochondria. Optimum balance between hydrophobicity and hydrophilicity is a critical factor for achieving self-assembly inside the mitochondria, thereby providing greater selectivity against cancer cells.

摘要

两亲性肽的细胞内或细胞周自组装正成为一种有前途的癌症治疗策略。由于复杂的细胞环境,包括许多可能改变合成肽自组装倾向的两亲性生物分子,因此实现在细胞或细胞器内进行两亲性肽的自组装具有挑战性。本文中,我们展示了两亲性肽的疏水性-亲水性平衡决定了自组装倾向,从而控制了细胞的命运。设计了一系列肽以靶向并在癌细胞的线粒体中自组装。通过改变 N 端封端来调整肽的疏水性。分析表明,最大疏水性的肽在到达线粒体之前就已自组装,对癌细胞没有选择性,而亲水性肽则不能在线粒体中自组装。疏水性和亲水性之间的最佳平衡是实现在线粒体中自组装的关键因素,从而提供了针对癌细胞的更高选择性。

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