STING Protein‐Based In Situ Vaccine Synergizes CD4<sup>+</sup> T, CD8<sup>+</sup> T, and NK Cells for Tumor Eradication

He, Yanpu; Hong, Celestine; Huang, Shengnan; Kaskow, Justin A.; Covarrubias, Gil; Pires, Ivan S.; Sacane, James C.; Hammond, Paula T.; Belcher, Angela M.

doi:10.1002/adhm.202300688

Cited by 2 publications

References 82 publications

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Extracellular Matrix Scaffold‐Assisted Tumor Vaccines Induce Tumor Regression and Long‐Term Immune Memory

Pal,

Chaudhari,

Baurceanu

et al. 2024

Advanced Materials

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Injectable scaffold delivery is a strategy to enhance the efficacy of cancer vaccine immunotherapy. The choice of scaffold biomaterial is crucial, impacting both vaccine release kinetics and immune stimulation via the host response. Extracellular matrix (ECM) scaffolds prepared from decellularized tissues facilitate a pro‐healing inflammatory response that promotes local cancer immune surveillance. Here, we engineered an ECM scaffold‐assisted therapeutic cancer vaccine that maintained an immune microenvironment consistent with tissue reconstruction. Several immune‐stimulating adjuvants were screened to develop a cancer vaccine formulated with decellularized small intestinal submucosa ECM scaffold co‐delivery. We found that the STING pathway agonist CDA most effectively induced cytotoxic immunity in an ECM scaffold vaccine, without compromising key IL‐4 mediated immune pathways associated with healing. ECM scaffold delivery enhanced therapeutic vaccine efficacy, curing 50–75% of established EG.7 lymphoma tumors in mice, while none were cured with soluble vaccine. SIS‐ECM scaffold‐assisted vaccination prolonged antigen exposure, was dependent on CD8+ cytotoxic T cells, and generated long‐term antigen‐specific immune memory for at least 10 months post‐vaccination. This study shows that an ECM scaffold is a promising delivery vehicle to enhance cancer vaccine efficacy while being orthogonal to characteristics of pro‐healing immune hallmarks.This article is protected by copyright. All rights reserved

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Extracellular Matrix Scaffold‐Assisted Tumor Vaccines Induce Tumor Regression and Long‐Term Immune Memory

Pal,

Chaudhari,

Baurceanu

et al. 2024

Advanced Materials

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Extracellular matrix scaffold-assisted tumor vaccines induce tumor regression and long-term immune memory

Pal,

Chaudhari,

Baurceanu

et al. 2023

Preprint

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Injectable scaffold delivery is an immune engineering strategy to enhance the efficacy and reliability of cancer vaccine immunotherapy. The composition and structure of the biomaterial scaffold determines both vaccine release kinetics and inherent immune stimulation via the scaffold host response. Extracellular matrix (ECM) scaffolds prepared from decellularized tissues initiate an acute alternative inflammatory response following implantation, which facilitates wound healing following tumor resection and promotes local cancer immune surveillance. However, it remains unknown whether this environment is compatible with generating protective anti-tumor cytotoxic immunity with local immunotherapy delivery. Here, we engineered an ECM scaffold-assisted therapeutic cancer vaccine that maintained an immune microenvironment consistent with tissue reconstruction. Immune adjuvants MPLA, GM-CSF, and CDA were screened in a cancer vaccine formulated for decellularized small intestinal submucosa (SIS) ECM scaffold co-delivery. Though MPLA and GM-CSF showed the greatest increase in local myeloid cell infiltration, we found that the STING pathway adjuvant CDA was the most potent inducer of cytotoxic immunity with SIS-ECM scaffold delivery. Further, CDA did not diminish hallmark ECM immune responses needed in wound healing such as high Il4 cytokine expression. SIS scaffold delivery enhanced therapeutic vaccine efficacy using CDA and the antigen ovalbumin, curing greater than 50% of established EG.7 tumors in young mice and 75% in 24-week-old mature mice, compared to soluble components alone (0% cured). SIS-ECM scaffold assisted vaccination extended antigen exposure, was dependent on CD8+ cytotoxic T cells, and generated long term anti-tumor memory at least 7 months post-vaccination in both young and mature-aged mice. This study shows that an ECM scaffold is a promising delivery vehicle to enhance cancer vaccine efficacy while being orthogonal to characteristics of pro-healing immune hallmarks.

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STING Protein‐Based In Situ Vaccine Synergizes CD4⁺ T, CD8⁺ T, and NK Cells for Tumor Eradication

Cited by 2 publications

References 82 publications

Extracellular Matrix Scaffold‐Assisted Tumor Vaccines Induce Tumor Regression and Long‐Term Immune Memory

Extracellular Matrix Scaffold‐Assisted Tumor Vaccines Induce Tumor Regression and Long‐Term Immune Memory

Extracellular matrix scaffold-assisted tumor vaccines induce tumor regression and long-term immune memory

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STING Protein‐Based In Situ Vaccine Synergizes CD4+ T, CD8+ T, and NK Cells for Tumor Eradication

Cited by 2 publications

References 82 publications

Extracellular Matrix Scaffold‐Assisted Tumor Vaccines Induce Tumor Regression and Long‐Term Immune Memory

Extracellular Matrix Scaffold‐Assisted Tumor Vaccines Induce Tumor Regression and Long‐Term Immune Memory

Extracellular matrix scaffold-assisted tumor vaccines induce tumor regression and long-term immune memory

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STING Protein‐Based In Situ Vaccine Synergizes CD4⁺ T, CD8⁺ T, and NK Cells for Tumor Eradication