4.6 Article

The effect of PEGylation on the efficacy and uptake of an immunostimulatory nanoparticle in the tumor immune microenvironment

NANOSCALE ADVANCES (2021)

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Journal

NANOSCALE ADVANCES
Volume 3, Issue 17, Pages 4961-4972

Publisher

ROYAL SOC CHEMISTRY
DOI: 10.1039/d1na00308a

Keywords

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Categories

Chemistry, Multidisciplinary Nanoscience & Nanotechnology Materials Science, Multidisciplinary

Funding

  1. National Cancer Institute [R01CA253627, U01CA198892]
  2. Case Comprehensive Cancer Center Support Grant [P30CA043703]
  3. Clinical Translational Science Collaborative of Cleveland [UL1TR002548]
  4. NSF graduate research fellowships program
  5. NIH Interdisciplinary Biomedical Imaging Training Program [T32EB007509]
  6. Shiverick Family Fund

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Immunostimulatory silica mesoporous nanoparticles (immuno-MSN) were developed to reprogram tumor-resident innate immune cells and enhance interferon production. The degree of PEGylation significantly influenced the uptake of 'empty' MSNs by tumor-resident innate immune cells, but not for the agonist-loaded immuno-MSN variants. Finding a balance between immune evasion and uptake by target immune cells is key in designing PEGylated immunostimulatory nanoparticles.
The efficacy of immunotherapies is often limited by the immunosuppressive tumor microenvironment, which is populated with dysfunctional innate immune cells. To reprogram the tumor-resident innate immune cells, we developed immunostimulatory silica mesoporous nanoparticles (immuno-MSN). The cargo of immuno-MSN is a Stimulator of Interferon Gene (STING) agonist, which activates innate immune cells leading to production of interferon (IFN) beta. By proficiently trafficking its cargo into immune cells, the immuno-MSN induced a 9-fold increase of IFN-beta secretion compared to free agonist. While an external PEG shield has historically been used to protect nanoparticles from immune recognition, a PEGylated immunostimulatory nanoparticle needs to strike a balance between immune evasion to avoid off-site accumulation and uptake by target immune cells in tumors. Using the 4T1 mouse model of metastatic breast cancer and flow cytometry, it was determined that the degree of PEGylation significantly influenced the uptake of 'empty' MSNs by tumor-resident innate immune cells. This was not the case for the agonist-loaded immuno-MSN variants. It should be noted the surface charge of the 'empty' MSNs was positive rather than neutral for the agonist-loaded immuno-MSNs. However, even though the cellular uptake was similar at 24 h after injection for the three immuno-MSN variants, we observed a significant beneficial effect on the activation and expansion of APCs especially in lung metastasis using the lightly PEGylated immuno-MSN variant.

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