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In Situ Self-Sorting Peptide Assemblies in Living Cells for Simultaneous Organelle Targeting

细胞器 化学 高尔基体 内质网 细胞生物学 赫拉 生物物理学 细胞 生物化学 生物
作者
Xin Liu,Mingming Li,Juanzu Liu,Yanqiu Song,Binbin Hu,Chunxia Wu,An-an Liu,Hao Zhou,Jiafu Long,Linqi Shi,Zhilin Yu
出处
期刊:Journal of the American Chemical Society [American Chemical Society]
卷期号:144 (21): 9312-9323 被引量:20
标识
DOI:10.1021/jacs.2c01025
摘要

Self-sorting is a common phenomenon in eukaryotic cells and represents one of the versatile strategies for the formation of advanced functional materials; however, developing artificial self-sorting assemblies within living cells remains challenging. Here, we report on the GSH-responsive in situ self-sorting peptide assemblies within cancer cells for simultaneous organelle targeting to promote combinatorial organelle dysfunction and thereby cell death. The self-sorting system was created via the design of two peptides E3C16E6 and EVMSeO derived from lipid-inspired peptide interdigitating amphiphiles and peptide bola-amphiphiles, respectively. The distinct organization patterns of the two peptides facilitate their GSH-induced self-sorting into isolated nanofibrils as a result of cleavage of disulfide-connected hydrophilic domains or reduction of selenoxide groups. The GSH-responsive in situ self-sorting in the peptide assemblies within HeLa cells was directly characterized by super-resolution structured illumination microscopy. Incorporation of the thiol and ER-targeting groups into the self-sorted assemblies endows their simultaneous targeting of endoplasmic reticulum and Golgi apparatus, thus leading to combinatorial organelle dysfunction and cell death. Our results demonstrate the establishment of the in situ self-sorting peptide assemblies within living cells, thus providing a unique platform for drug targeting delivery and an alternative strategy for modulating biological processes in the future.
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