| Literature DB >> 33644299 |
Ching-Hsin Huang1, Natalie Mendez1, Oscar Hernandez Echeagaray2, Joi Weeks2, James Wang1, Shiyin Yao3, Sarah L Blair3, Natalie Gude2, William C Trogler1, Dennis A Carson3, Tomoko Hayashi3, Andrew C Kummel1.
Abstract
Mono- or dual-checkpoint inhibitors for immunotherapy have changed the paradigm of cancer care; however, only a minority of patients responds to such treatment. Combining small molecule immuno-stimulators can improve treatment efficacy, but they are restricted by poor pharmacokinetics. In this study, TLR7 agonists conjugated onto silica nanoparticles showed extended drug localization after intratumoral injection. The nanoparticle-based TLR7 agonist increased immune stimulation by activating the TLR7 signaling pathway. When treating CT26 colon cancer, nanoparticle conjugated TLR7 agonists increased T cell infiltration into the tumors by > 4× and upregulated expression of the interferon γ gene compared to its unconjugated counterpart by ~2×. Toxicity assays established that the conjugated TLR7 agonist is a safe agent at the effective dose. When combined with checkpoint inhibitors that target programmed cell death protein 1 (PD-1) and cytotoxic T-lymphocyte-associated protein 4 (CTLA-4), a 10-100× increase in immune cell migration was observed; furthermore, 100 mm3 tumors were treated and a 60% remission rate was observed including remission at contralateral non-injected tumors. The data show that nanoparticle based TLR7 agonists are safe and can potentiate the effectiveness of checkpoint inhibitors in immunotherapy resistant tumor models and promote a long-term specific memory immune function.Entities:
Year: 2020 PMID: 33644299 PMCID: PMC7904104 DOI: 10.1002/adtp.201900200
Source DB: PubMed Journal: Adv Ther (Weinh) ISSN: 2366-3987