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Enzyme-instructed and mitochondria-targeting peptide self-assembly to efficiently induce immunogenic cell death

Debin Zheng, Jingfei Liu, Li‐Min Xie, Yuhan Wang, Yinghao Ding, Rong Peng, Min Cui, Ling Wang, Yongjie Zhang, Chunqiu Zhang, Zhimou Yang

2021Acta Pharmaceutica Sinica B49 citationsDOIOpen Access PDF

Abstract

Immunogenic cell death (ICD) plays a major role in cancer immunotherapy by stimulating specific T cell responses and restoring the antitumor immune system. However, effective type II ICD inducers without biotoxicity are still very limited. Herein, a tentative drug- or photosensitizer-free strategy was developed by employing enzymatic self-assembly of the peptide F-pY-T to induce mitochondrial oxidative stress in cancer cells. Upon dephosphorylation catalyzed by alkaline phosphatase overexpressed on cancer cells, the peptide F-pY-T self-assembled to form nanoparticles, which were subsequently internalized. These affected the morphology of mitochondria and induced serious reactive oxygen species production, causing the ICD characterized by the release of danger-associated molecular patterns (DAMPs). DAMPs enhanced specific immune responses by promoting the maturation of DCs and the intratumoral infiltration of tumor-specific T cells to eradicate tumor cells. The dramatic immunotherapeutic capacity could be enhanced further by combination therapy of F-pY-T and anti-PD-L1 agents without visible biotoxicity in the main organs. Thus, our results revealed an alternative strategy to induce efficient ICD by physically promoting mitochondrial oxidative stress.

Topics & Concepts

Immunogenic cell deathDephosphorylationMitochondrionProgrammed cell deathImmune systemCancer cellChemistryReactive oxygen speciesOxidative stressCell biologyCancer immunotherapyImmunotherapyPeptideCytotoxic T cellCancer researchEnzymeApoptosisBiochemistryCancerPhosphataseBiologyImmunologyIn vitroGeneticsNanoplatforms for cancer theranosticsPeptidase Inhibition and AnalysisAdenosine and Purinergic Signaling
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