Issue 19, 2023

Tuning innate immune function using microneedles containing multiple classes of toll-like receptor agonists

Abstract

Microneedle arrays (MNAs) are patches displaying hundreds of micron-scale needles that can penetrate skin. As a result, these arrays efficiently and painlessly access this immune cell-rich niche, motivating significant clinical interest in MNA-based vaccines. Our lab has developed immune polyelectrolyte multilayers (iPEMs), nanostructures built entirely from immune signals employing electrostatic self-assembly. iPEMs consist of positively charged peptide antigen and negatively charged toll-like receptor agonists (TLRas) to assemble these components at ultra-high density since no carrier is needed. Here we used this technology to deliver MNAs with antigen and defined ratios of multiple classes of TLRa. Notably, this approach resulted in facile assembly and corresponding signal transduction through each respective TLR pathway. This control ultimately activated primary antigen presenting cells and drove proliferation of antigen-specific T cells. In related in vivo vaccine studies, application of MNAs resulted in distinct T cells response depending on the number of TLRa classes delivered with MNAs. These MNAs technologies create an opportunity to deliver nanostructured vaccine components at high density, and to probe integration of multiple TLRas in skin to tune immunity.

Graphical abstract: Tuning innate immune function using microneedles containing multiple classes of toll-like receptor agonists

Supplementary files

Article information

Article type
Paper
Submitted
21 Urt. 2023
Accepted
19 Api. 2023
First published
25 Api. 2023

Nanoscale, 2023,15, 8662-8674

Tuning innate immune function using microneedles containing multiple classes of toll-like receptor agonists

C. Edwards, R. S. Oakes and C. M. Jewell, Nanoscale, 2023, 15, 8662 DOI: 10.1039/D3NR00333G

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