Delivery to, and Reactivation of, the p53 Pathway in Cancer Cells Using a Grafted Cyclotide Conjugated with a Cell-Penetrating Peptide

被引:9
|
作者
Philippe, Gregoire Jean-Baptiste [1 ,2 ]
Huang, Yen-Hua [1 ]
Mittermeier, Anna [3 ]
Brown, Christopher J. [4 ]
Kaas, Quentin [1 ]
Ramlan, Siti Radhiah [4 ]
Wang, Conan K. [1 ]
Lane, David [4 ]
Loewer, Alexander [3 ]
Troeira Henriques, Sonia [2 ]
Craik, David J. [1 ]
机构
[1] Univ Queensland, Inst Mol Biosci, Australian Res Council Ctr Excellence Innovat Pep, Brisbane, Qld 4072, Australia
[2] Queensland Univ Technol, Translat Res Inst, Sch Biomed Sci, Brisbane, Qld 4102, Australia
[3] Tech Univ Darmstadt, Dept Biol, D-64287 Darmstadt, Germany
[4] ASTAR, Inst Mol & Cell Biol IMCB, Singapore 138673, Singapore
基金
英国医学研究理事会; 澳大利亚研究理事会; 澳大利亚国家健康与医学研究理事会;
关键词
MCOTI-II; PROTEIN; MDM2; SCAFFOLD; DESIGN; FAMILY; ONCOGENESIS; INHIBITION; ANTAGONIST; ACTIVATION;
D O I
10.1021/acs.jmedchem.3c01682
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Peptides are promising drug modalities that can modulate protein-protein interactions, but their application is hampered by their limited ability to reach intracellular targets. Here, we improved the cytosolic delivery of a peptide blocking p53:MDM2/X interactions using a cyclotide as a stabilizing scaffold. We applied several design strategies to improve intracellular delivery and found that the conjugation of the lead cyclotide to the cyclic cell-penetrating peptide cR10 was the most effective. Conjugation allowed cell internalization at micromolar concentration and led to elevated intracellular p53 levels in A549, MCF7, and MCF10A cells, as well as inducing apoptosis in A549 cells without causing membrane disruption. The lead peptide had >35-fold improvement in inhibitory activity and increased cellular uptake compared to a previously reported cyclotide p53 activator. In summary, we demonstrated the delivery of a large polar cyclic peptide in the cytosol and confirmed its ability to modulate intracellular protein-protein interactions involved in cancer.
引用
收藏
页码:1197 / 1208
页数:12
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