Lysosome-Instructed Self-Assembly of Amino-Acid-Functionalized Perylene Diimide for Multidrug-Resistant Cancer Cells.
Changjoon KeumJiyoung HongDoyeon KimSang-Yup LeeHyuncheol KimPublished in: ACS applied materials & interfaces (2021)
Multidrug resistance (MDR) of cancer cells reduces chemotherapeutic efficacy by preventing drug accumulation in the cells through a drug efflux pump and lysosomal sequestration/exocytosis. Herein, to overcome such anticancer resistance, lysosome-targeted self-assembly of perylene diimide (PDI) derivatives is presented as a powerful strategy for effective and selective anticancer therapy. Stimulated by the lysosomal low pH, the amphiphilic PDI derivatives functionalized with amino acids (PDI-AAs) construct fibrous self-assembled structures inside the lysosomes, causing cancer cell apoptosis by lysosomal rupture. In contrast, negligible apoptosis was observed from normal cells by PDI-AA. The agglomerated fibrous assemblies were not removed by lysosomal exocytosis, thereby displaying a 10.7-fold higher anticancer efficacy on MDR cancer cells compared to a doxorubicin chemotherapeutic agent. The MDR-circumventing capability, along with high selectivity toward cancer cells, supports PDI-AAs as potential candidates for the treatment of MDR cancer cells by lysosome-targeted self-assembly.
Keyphrases
- multidrug resistant
- cell cycle arrest
- amino acid
- induced apoptosis
- drug resistant
- acinetobacter baumannii
- gram negative
- endoplasmic reticulum stress
- fluorescent probe
- cancer therapy
- living cells
- klebsiella pneumoniae
- oxidative stress
- pi k akt
- cell proliferation
- stem cells
- magnetic resonance
- drug delivery
- papillary thyroid
- high resolution
- magnetic resonance imaging
- squamous cell carcinoma
- computed tomography
- climate change
- pseudomonas aeruginosa
- adverse drug
- mass spectrometry
- molecularly imprinted
- squamous cell