| Literature DB >> 32913042 |
Ziyang Xu1,2, Neethu Chokkalingam1, Edgar Tello-Ruiz1, Megan C Wise3, Mamadou A Bah1, Susanne Walker1, Nicholas J Tursi1, Paul D Fisher3, Katherine Schultheis3, Kate E Broderick3, Laurent Humeau3, Daniel W Kulp4, David B Weiner4.
Abstract
Cytolytic T cells (CTL) play a pivotal role in surveillance against tumors. Induction of CTL responses by vaccination may be challenging, as it requires direct transduction of target cells or special adjuvants to promote cross-presentation. Here, we observed induction of robust CTL responses through electroporation-facilitated, DNA-launched nanoparticle vaccination (DLnano-vaccines). Electroporation was observed to mediate transient tissue apoptosis and macrophage infiltration, which were deemed essential to the induction of CTLs by DLnano-vaccines through a systemic macrophage depletion study. Bolus delivery of protein nano-vaccines followed by electroporation, however, failed to induce CTLs, suggesting direct in vivo production of nano-vaccines may be required. Following these observations, new DLnano-vaccines scaffolding immunodominant melanoma Gp100 and Trp2 epitopes were designed and shown to induce more potent and consistent epitope-specific CTL responses than the corresponding DNA monomeric vaccines or CpG-adjuvanted peptide vaccines. DNA, but not recombinant protein, nano-vaccinations induced CTL responses to these epitopes and suppressed melanoma tumor growth in mouse models in a CD8+ T-cell-dependent fashion. Further studies to explore the use of DLnano-vaccines against other cancer targets and the biology with which they induce CTLs are important. ©2020 American Association for Cancer Research.Entities:
Year: 2020 PMID: 32913042 PMCID: PMC7642117 DOI: 10.1158/2326-6066.CIR-20-0061
Source DB: PubMed Journal: Cancer Immunol Res ISSN: 2326-6066 Impact factor: 11.151