Three‐in‐One Peptide Prodrug with Targeting, Assembly and Release Properties for Overcoming Bacterium‐Induced Drug Resistance and Potentiating Anti‐Cancer Immune Response

Author:

Gao Ge123ORCID,Jiang Yao‐Wen4,Chen Jiaxuan123,Xu Xiaodi123,Sun Xianbao5,Xu Haidong5,Liang Gaolin5,Liu Xiaoyang5,Zhan Wenjun5,Wang Meng123,Xu Yixin6,Zheng Junnian123,Wang Gang123

Affiliation:

1. Cancer Institute Xuzhou Medical University 209 Tongshan Road Xuzhou Jiangsu 221004 China

2. Center of Clinical Oncology The Affiliated Hospital of Xuzhou Medical University 99 Huaihai Road Xuzhou Jiangsu 221002 China

3. Jiangsu Center for the Collaboration and Innovation of Cancer Biotherapy Xuzhou Medical University 209 Tongshan Road Xuzhou Jiangsu 221004 China

4. School of Medical Imaging Xuzhou Medical University 209 Tongshan Road Xuzhou Jiangsu 221004 China

5. State Key Laboratory of Bioelectronics School of Biological Science and Medical Engineering Southeast University Nanjing Jiangsu 210096 China

6. Department of General Surgery Affiliated Hospital of Xuzhou Medical University Xuzhou 221000 China

Abstract

AbstractThe presence of bacteria in tumor results in chemotherapeutic drug resistance and weakens the immune response in colorectal cancer. To overcome bacterium‐induced chemotherapeutic drug resistance and potentiate antitumor immunity, herein a novel molecule Biotin‐Lys(SA‐Cip‐OH)‐Lys(SA‐CPT)‐Phe‐Phe‐Nap (Biotin‐Cip‐CPT‐Nap) is rationally designed containing four functional motifs (i.e., a biotin motif for targeting, Phe‐Phe(‐Nap) motif for self‐assembly, ciprofloxacin derivative (Cip‐OH) motif for antibacterial effect, and camptothecin (CPT) motif for chemotherapy). Using the designed molecule, a novel strategy of intracellular enzymatic nanofiber formation and synergistic antibacterium‐enhanced chemotherapy and immunotherapy is achieved. Under endocytosis mediated by highly expressed biotin receptor in colorectal cancer cell membrane and the catalysis of highly expressed carboxylesterase in the cytoplasm, this novel molecule can be transformed into Biotin‐Nap, which self‐assembled into nanofibers. Meanwhile, antibiotic Cip‐OH and chemotherapeutic drug CPT are released, overcoming bacterium‐induced drug resistance and enhancing the therapeutic efficacy of immunotherapy towards colorectal cancer. This work offers a feasible strategy for the design of novel multifunctional prodrugs to improve the efficiency of colorectal cancer treatment.

Funder

National Key Research and Development Program of China

National Natural Science Foundation of China

Natural Science Foundation of Jiangsu Province

Publisher

Wiley

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