Noncovalently particle-anchored cytokines with prolonged tumor retention safely elicit potent antitumor immunity

Liqian Niu; Eungyo Jang; Ai Lin Chin; Ziyu Huo; Wenbo Wang; Wenjun Cai; Rong Tong

doi:10.1126/sciadv.adk7695

Noncovalently particle-anchored cytokines with prolonged tumor retention safely elicit potent antitumor immunity

Liqian Niu, Eungyo Jang, Ai Lin Chin, Ziyu Huo, Wenbo Wang, Wenjun Cai, Rong Tong

Surface Engineering and Tribology

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

1 Scopus citations

Abstract

Preclinical studies have shown that immunostimulatory cytokines elicit antitumor immune responses but their clinical use is limited by severe immune-related adverse events upon systemic administration. Here, we report a facile and versatile strategy for noncovalently anchoring potent Fc-fused cytokine molecules to the surface of size-discrete particles decorated with Fc-binding peptide for local administration. Following intratumoral injection, particle-anchored Fc cytokines exhibit size-dependent intratumoral retention. The 1-micrometer particle prolongs intratumoral retention of Fc cytokine for over a week and has minimal systemic exposure, thereby eliciting antitumor immunity while eliminating systemic toxicity caused by circulating cytokines. In addition, the combination of these particle-anchored cytokines with immune checkpoint blockade antibodies safely promotes tumor regression in various syngeneic tumor models and genetically engineered murine tumor models and elicits systemic antitumor immunity against tumor rechallenge. Our formulation strategy renders a safe and tumor-agnostic approach that uncouples cytokines’ immunostimulatory properties from their systemic toxicities for potential clinical application.

Original language	English
Article number	eadk7695
Journal	Science Advances
Volume	10
Issue number	16
DOIs	https://doi.org/10.1126/sciadv.adk7695
State	Published - Apr 2024

Funding

Acknowledgments: We are grateful to M. Makris (college of veterinary Medicine, virginia tech) for help on flow cytometry. Funding: this work was supported by the Jeffress trust Awards and the National Science Foundation (che-1807911 to R.t.). Author contributions: conceptualization: l.N. and R.t. Methodology: l.N., e.J., A.l.c., W.W., W.c., and R.t. investigation: l.N., e.J., A.l.c., W.W., W.c., and R.t. visualization: l.N., Z.h., and R.t. Supervision: R.t. Writing\u2014original draft: l.N. and R.t. Writing\u2014review and editing: l.N. and R.t. Competing interests: the authors declare that they have no competing interests. Data and materials availability: All data needed to evaluate the conclusions in the paper are present in the paper and/or the Supplementary Materials (data are accessible through the virginia tech data Repository at https://doi.org/10.7294/25315681).

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title = "Noncovalently particle-anchored cytokines with prolonged tumor retention safely elicit potent antitumor immunity",

abstract = "Preclinical studies have shown that immunostimulatory cytokines elicit antitumor immune responses but their clinical use is limited by severe immune-related adverse events upon systemic administration. Here, we report a facile and versatile strategy for noncovalently anchoring potent Fc-fused cytokine molecules to the surface of size-discrete particles decorated with Fc-binding peptide for local administration. Following intratumoral injection, particle-anchored Fc cytokines exhibit size-dependent intratumoral retention. The 1-micrometer particle prolongs intratumoral retention of Fc cytokine for over a week and has minimal systemic exposure, thereby eliciting antitumor immunity while eliminating systemic toxicity caused by circulating cytokines. In addition, the combination of these particle-anchored cytokines with immune checkpoint blockade antibodies safely promotes tumor regression in various syngeneic tumor models and genetically engineered murine tumor models and elicits systemic antitumor immunity against tumor rechallenge. Our formulation strategy renders a safe and tumor-agnostic approach that uncouples cytokines{\textquoteright} immunostimulatory properties from their systemic toxicities for potential clinical application.",

author = "Liqian Niu and Eungyo Jang and Chin, {Ai Lin} and Ziyu Huo and Wenbo Wang and Wenjun Cai and Rong Tong",

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AU - Wang, Wenbo

AU - Cai, Wenjun

AU - Tong, Rong

PY - 2024/4

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N2 - Preclinical studies have shown that immunostimulatory cytokines elicit antitumor immune responses but their clinical use is limited by severe immune-related adverse events upon systemic administration. Here, we report a facile and versatile strategy for noncovalently anchoring potent Fc-fused cytokine molecules to the surface of size-discrete particles decorated with Fc-binding peptide for local administration. Following intratumoral injection, particle-anchored Fc cytokines exhibit size-dependent intratumoral retention. The 1-micrometer particle prolongs intratumoral retention of Fc cytokine for over a week and has minimal systemic exposure, thereby eliciting antitumor immunity while eliminating systemic toxicity caused by circulating cytokines. In addition, the combination of these particle-anchored cytokines with immune checkpoint blockade antibodies safely promotes tumor regression in various syngeneic tumor models and genetically engineered murine tumor models and elicits systemic antitumor immunity against tumor rechallenge. Our formulation strategy renders a safe and tumor-agnostic approach that uncouples cytokines’ immunostimulatory properties from their systemic toxicities for potential clinical application.

AB - Preclinical studies have shown that immunostimulatory cytokines elicit antitumor immune responses but their clinical use is limited by severe immune-related adverse events upon systemic administration. Here, we report a facile and versatile strategy for noncovalently anchoring potent Fc-fused cytokine molecules to the surface of size-discrete particles decorated with Fc-binding peptide for local administration. Following intratumoral injection, particle-anchored Fc cytokines exhibit size-dependent intratumoral retention. The 1-micrometer particle prolongs intratumoral retention of Fc cytokine for over a week and has minimal systemic exposure, thereby eliciting antitumor immunity while eliminating systemic toxicity caused by circulating cytokines. In addition, the combination of these particle-anchored cytokines with immune checkpoint blockade antibodies safely promotes tumor regression in various syngeneic tumor models and genetically engineered murine tumor models and elicits systemic antitumor immunity against tumor rechallenge. Our formulation strategy renders a safe and tumor-agnostic approach that uncouples cytokines’ immunostimulatory properties from their systemic toxicities for potential clinical application.

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Noncovalently particle-anchored cytokines with prolonged tumor retention safely elicit potent antitumor immunity

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