Cascaded immunotherapy with implantable dual-drug depots sequentially releasing STING agonists and apoptosis inducers

Kai Li; Xuan Yu; Yanteng Xu; Haixia Wang; Zheng Liu; Chong Wu; Xing Luo; Jiancheng Xu; Youqiang Fang; Enguo Ju; Shixian Lv; Hon Fai Chan; Yeh Hsing Lao; Weiling He; Yu Tao; Mingqiang Li

doi:10.1038/s41467-025-56407-7

Cascaded immunotherapy with implantable dual-drug depots sequentially releasing STING agonists and apoptosis inducers

Kai Li
, Xuan Yu
, Yanteng Xu
, Haixia Wang
, Zheng Liu
, Chong Wu
, Xing Luo
, Jiancheng Xu
, Youqiang Fang
, Enguo Ju
, Shixian Lv
, Hon Fai Chan
, Yeh Hsing Lao
, Weiling He
, Yu Tao
, Mingqiang Li

Pharmaceutical Sciences

Sun Yat-Sen University
Xiang’an Hospital of Xiamen University; Fujian Provincial Key Laboratory of Ophthalmology and Visual Science; Fujian Engineering and Research Center of Eye Regenerative Medicine; Eye Institute of Xiamen University; School of Medicine
Peking University
Chinese University of Hong Kong
Guangdong Provincial Key Laboratory of Liver Disease Research

Research output: Contribution to journal › Article › peer-review

27 Scopus citations

Abstract

Non-nucleotide stimulators of interferon gene (STING) agonists hold promise as immunotherapeutic agents for postsurgical adjuvant treatment of tumors. However, their limited effect duration hampers therapeutic effectiveness, necessitating prolonged administration of multiple doses that heightens infection risk and impacts patient compliance. Here, we develop an implantable dual-drug depot in a sandwich-like configuration, with a non-nucleotide STING agonist (MSA-2) in the outer layers of 3D-printed scaffolds and an immunogenic apoptosis inducer (doxorubicin, DOX) in the inner layer of electrospun fibers. We discover that MSA-2 can elicit endoplasmic reticulum stress-mediated and general immunogenic apoptosis of cancer cells. The stimulations with tumor-associated antigens and damage-associated molecular patterns from cancer cells, along with proinflammatory factors secreted by matured dendritic cells and M1-polarized macrophages, can depolymerize intracellular microtubules guiding activated STING trafficking towards lysosomes for degradation. Collectively, the dual-drug depots can initiate a long-lasting cascaded immunotherapy and chemotherapy, suppressing postsurgical tumor recurrence and metastasis.

Original language	English
Article number	1629
Journal	Nature Communications
Volume	16
Issue number	1
DOIs	https://doi.org/10.1038/s41467-025-56407-7
State	Published - Dec 2025

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title = "Cascaded immunotherapy with implantable dual-drug depots sequentially releasing STING agonists and apoptosis inducers",

abstract = "Non-nucleotide stimulators of interferon gene (STING) agonists hold promise as immunotherapeutic agents for postsurgical adjuvant treatment of tumors. However, their limited effect duration hampers therapeutic effectiveness, necessitating prolonged administration of multiple doses that heightens infection risk and impacts patient compliance. Here, we develop an implantable dual-drug depot in a sandwich-like configuration, with a non-nucleotide STING agonist (MSA-2) in the outer layers of 3D-printed scaffolds and an immunogenic apoptosis inducer (doxorubicin, DOX) in the inner layer of electrospun fibers. We discover that MSA-2 can elicit endoplasmic reticulum stress-mediated and general immunogenic apoptosis of cancer cells. The stimulations with tumor-associated antigens and damage-associated molecular patterns from cancer cells, along with proinflammatory factors secreted by matured dendritic cells and M1-polarized macrophages, can depolymerize intracellular microtubules guiding activated STING trafficking towards lysosomes for degradation. Collectively, the dual-drug depots can initiate a long-lasting cascaded immunotherapy and chemotherapy, suppressing postsurgical tumor recurrence and metastasis.",

author = "Kai Li and Xuan Yu and Yanteng Xu and Haixia Wang and Zheng Liu and Chong Wu and Xing Luo and Jiancheng Xu and Youqiang Fang and Enguo Ju and Shixian Lv and Chan, \{Hon Fai\} and Lao, \{Yeh Hsing\} and Weiling He and Yu Tao and Mingqiang Li",

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AU - Li, Kai

AU - Yu, Xuan

AU - Xu, Yanteng

AU - Wang, Haixia

AU - Liu, Zheng

AU - Wu, Chong

AU - Luo, Xing

AU - Xu, Jiancheng

AU - Fang, Youqiang

AU - Ju, Enguo

AU - Lv, Shixian

AU - Chan, Hon Fai

AU - Lao, Yeh Hsing

AU - He, Weiling

AU - Tao, Yu

AU - Li, Mingqiang

PY - 2025/12

Y1 - 2025/12

N2 - Non-nucleotide stimulators of interferon gene (STING) agonists hold promise as immunotherapeutic agents for postsurgical adjuvant treatment of tumors. However, their limited effect duration hampers therapeutic effectiveness, necessitating prolonged administration of multiple doses that heightens infection risk and impacts patient compliance. Here, we develop an implantable dual-drug depot in a sandwich-like configuration, with a non-nucleotide STING agonist (MSA-2) in the outer layers of 3D-printed scaffolds and an immunogenic apoptosis inducer (doxorubicin, DOX) in the inner layer of electrospun fibers. We discover that MSA-2 can elicit endoplasmic reticulum stress-mediated and general immunogenic apoptosis of cancer cells. The stimulations with tumor-associated antigens and damage-associated molecular patterns from cancer cells, along with proinflammatory factors secreted by matured dendritic cells and M1-polarized macrophages, can depolymerize intracellular microtubules guiding activated STING trafficking towards lysosomes for degradation. Collectively, the dual-drug depots can initiate a long-lasting cascaded immunotherapy and chemotherapy, suppressing postsurgical tumor recurrence and metastasis.

AB - Non-nucleotide stimulators of interferon gene (STING) agonists hold promise as immunotherapeutic agents for postsurgical adjuvant treatment of tumors. However, their limited effect duration hampers therapeutic effectiveness, necessitating prolonged administration of multiple doses that heightens infection risk and impacts patient compliance. Here, we develop an implantable dual-drug depot in a sandwich-like configuration, with a non-nucleotide STING agonist (MSA-2) in the outer layers of 3D-printed scaffolds and an immunogenic apoptosis inducer (doxorubicin, DOX) in the inner layer of electrospun fibers. We discover that MSA-2 can elicit endoplasmic reticulum stress-mediated and general immunogenic apoptosis of cancer cells. The stimulations with tumor-associated antigens and damage-associated molecular patterns from cancer cells, along with proinflammatory factors secreted by matured dendritic cells and M1-polarized macrophages, can depolymerize intracellular microtubules guiding activated STING trafficking towards lysosomes for degradation. Collectively, the dual-drug depots can initiate a long-lasting cascaded immunotherapy and chemotherapy, suppressing postsurgical tumor recurrence and metastasis.

UR - https://www.scopus.com/pages/publications/85218459790

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DO - 10.1038/s41467-025-56407-7

M3 - Article

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SN - 2041-1723

VL - 16

JO - Nature Communications

JF - Nature Communications

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ER -

Cascaded immunotherapy with implantable dual-drug depots sequentially releasing STING agonists and apoptosis inducers

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