Sequential delivery of photosensitizers and checkpoint inhibitors by engineered bacteria for enhanced cancer photodynamic immunotherapy

Author:

Liu Xinyu12,Fan Yali3,Zhang Xinyu12,Li Lianyue12,Yang Chao4,Ma Xiaoyan4,Bai Guijie12,Sun Dawei12,Wang Yaxin12,Wang Junyi12,Li Yong1,Shi Yanyan5,Liu Jing12,Zhang Yingying3,Wang Hanjie12ORCID

Affiliation:

1. School of Life Sciences Tianjin University Tianjin China

2. Tianjin Engineering Center of Micro‐Nano Biomaterials and Detection‐Treatment Technology Tianjin Key Laboratory of Function and Application of Biological Macromolecular Structures Tianjin China

3. School of Medical Imaging Xuzhou Medical University Xuzhou China

4. Key Laboratory of Molecular Medicine and Biotherapy, School of Life Science Beijing Institute of Technology Beijing China

5. Research Center of Clinical Epidemiology Peking University Third Hospital Beijing China

Abstract

AbstractEngineered bacteria‐based cancer therapy has increasingly been considered to be a promising therapeutic strategy due to the development of synthetic biology. Wherein, engineering bacteria‐mediated photodynamic therapy (PDT)‐immunotherapy shows greater advantages and potential in treatment efficiency than monotherapy. However, the unsustainable regeneration of photosensitizers (PSs) and weak immune responses limit the therapeutic efficiency. Herein, we developed an engineered bacteria‐based delivery system for sequential delivery of PSs and checkpoint inhibitors in cancer PDT‐immunotherapy. The biosynthetic pathway of 5‐aminolevulinic acid (5‐ALA) was introduced into Escherichia coli, yielding a supernatant concentration of 172.19 mg/L after 10 h of growth. And another strain was endowed with the light‐controllable releasement of anti‐programmed cell death‐ligand 1 nanobodies (anti‐PD‐L1). This system exhibited a collaborative effect, where PDT initiated tumor cell death and the released tumor cell fragments stimulated immunity, followed by the elimination of residual tumor cells. The tumor inhibition rate reached 74.97%, and the portion of activated T cells and inflammatory cytokines were reinforced. The results demonstrated that the engineered bacteria‐based collaborative system could sequentially deliver therapeutic substance and checkpoint inhibitors, and achieve good therapeutic therapy. This paper will provide a new perspective for the cancer PDT‐immunotherapy.

Publisher

Wiley

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