Hypoxia‐Responsive Tetrameric Supramolecular Polypeptide Nanoprodrugs for Combination Therapy

Author:

Ding Yue1ORCID,Yu Wei1,Shen Rongkai2,Zheng Xiangqin3,Zheng Hui3,Yao Yong1,Zhang Yuehua1,Du Chang4,Yi Huan3

Affiliation:

1. School of Chemistry and Chemical Engineering Nantong University Nantong 226019 P. R. China

2. Department of Orthopedics The First Affiliated Hospital of Fujian Medical University 20, Chazhong Rd. Fuzhou Fujian 350005 China

3. Fujian Maternity and Child Health Hospital College of Clinical Medicine for Obstetrics & Gynecology and Pediatrics Fujian Medical University, National Key Clinical Specialty Construction Program of (Gynecology), Fujian Province Key Clinical Specialty for Gynecology Fujian Maternity and Child Health Hospital Fuzhou Fujian 350001 China

4. State Key Laboratory of Systems Medicine for Cancer Shanghai Cancer Institute Ren Ji Hospital School of Medicine Shanghai Jiao Tong University Shanghai 200240 China

Abstract

AbstractDespite the intense progress of photodynamic and chemotherapy, however, they cannot prevent solid tumor invasion, metastasis, and relapse, along with inferior efficacy and severe side effects. The hypoxia‐responsive nanoprodrugs integrating photodynamic functions are highly sought to address the above‐mentioned problems and overcome the tumor hypoxia‐reduced efficacy. Herein, a hypoxia‐responsive tetrameric supramolecular polypeptide nanoprodrug (SPN‐TAPP‐PCB4) is constructed from the self‐assembly of tetrameric porphyrin‐central poly(l‐lysine‐azobenzene‐chlorambucil) (TAPP‐(PLL‐Azo‐CB)4) and an anionic water‐soluble [2]biphenyl‐extended‐pillar[6]arene (AWBpP6) via the synergy of hydrophobic, ππ stacking, and host–guest interactions. Upon laser irradiation, the central TAPP can convert oxygen to generate single oxygen (1O2) to kill tumor cells. Furthermore, under the acidic and PDT‐aggravated hypoxia tumor cell microenvironment, SPN‐TAPP‐PCB4 is rapidly disassembled, and then efficiently releases activated CB through the hypoxic‐responsive cleavage of azobenzene linkages. Both in vitro and in vivo biological studies showcase synergistic cancer‐killing actions between photodynamic therapy (PDT) and chemotherapy (CT) with negligible toxicity. Consequently, this supramolecular polypeptide nanoprodrug offers an effective strategy to design a hypoxia‐responsive nanoprodrug for a potential combo PDT‐CT transition.

Funder

National Key Clinical Specialty Discipline Construction Program of China

Publisher

Wiley

Subject

Pharmaceutical Science,Biomedical Engineering,Biomaterials

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