Manipulating the Crosstalk between Cancer and Immunosuppressive Cells with Phototherapeutic Gold‐Nanohut for Reprogramming Tumor Microenvironment

Author:

Cheng Hung‐Wei1,Lee Wei2,Hsu Fei‐Ting3,Lai Yen‐Ho2,Huang Shu‐Rou4,Lim Chris Seh Hong5,Lin Zhen‐Kai1,Hsu Shih‐Chao6,Chiang Chih‐Sheng278ORCID,Jeng Long‐Bin2910,Shyu Woei‐Cherng478,Chen San‐Yuan1711ORCID

Affiliation:

1. Department of Materials Science and Engineering National Yang Ming Chiao Tung University Hsinchu 30010 Taiwan

2. Cell Therapy Center China Medical University Hospital Taichung 40447 Taiwan

3. Department of Biological Science and Technology China Medical University Taichung 406040 Taiwan

4. Translational Medicine Research Center New Drug development Center and Department of Neurology China Medical University Hospital Taichung 40447 Taiwan

5. Department of Physician Assistant Studies School of Health and Rehabilitation Sciences MGH Institute Boston Massachusetts 02114 USA

6. Department of Surgery China Medical University Hospital Taichung 40447 Taiwan

7. Graduate Institute of Biomedical Science China Medical University Taichung 406040 Taiwan

8. Neuroscience and Brain Disease Center China Medical University Taichung 40447 Taiwan

9. Organ Transplantation Center China Medical University Hospital Taichung 40447 Taiwan

10. School of Medicine China Medical University Taichung 406040 Taiwan

11. School of Dentistry College of Dental Medicine Kaohsiung Medical University Kaohsiung 807 Taiwan

Abstract

AbstractPhotoimmunotherapy faces challenges due to insufficient intratumoral accumulation of photothermal agents and the reversion of the cancer‐immunity cycle during treatment. In this study, an anti‐PD‐L1‐immobilized magnetic gold nanohut, AuNH‐2‐Ab, with photoresponsive, thermosensitive, and immunomodulatory properties to effectively suppress the growth of primary tumors, elevate immunogenic cell death (ICD) levels, reverse the tumor immune microenvironment (TIME), and consequently inhibit metastases are developed. AuNH‐2‐Ab achieves high tumor accumulation (9.54% injected dose) following systemic administration, allowing the modulation of hyperthermia dose of over 50 °C in the tumor. By optimizing the hyperthermia dose, AuNH‐2‐Ab simultaneously target and eliminate cancer cells and tumor‐associated macrophages, thereby activating potent antitumor immunity without being compromised by immunosuppressive elements. Hyperthermia/pH induced morphological transformation of AuNH‐2‐Ab involving the detachment of the surface antibody for in situ PD‐L1 inhibition, and exposure of the inner fucoidan layer for natural killer (NK) cell activation. This precision photoimmunotherapy approach reprograms the TIME, significantly prolongs survival in a murine hepatocellular carcinoma model (Hep55.1c), and harnesses the synergistic effects of ICD production and checkpoint inhibitors by utilizing a single nanoplatform.

Funder

National Science and Technology Council

China Medical University

Publisher

Wiley

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