Toll-like Receptor 7/8 Agonists Exert Antitumor Effect in a Mouse Melanoma Model
Gheorghita Isvoranu, Mihaela Surcel, Ana-Maria Enciu, Adriana Narcisa Munteanu, Monica Neagu, Andrei Marian Niculae, Gabriela Chiritoiu, Cristian V. A. Munteanu, Marioara Chiritoiu-Butnaru

TL;DR
This study shows that TLR7/8 agonists like imiquimod and gardiquimod can reduce melanoma tumor growth and activate immune cells in mice.
Contribution
The study demonstrates the antitumor efficacy of TLR7/8 agonists in a melanoma mouse model and compares their potency.
Findings
Both imiquimod and gardiquimod inhibited melanoma tumor growth in mice.
Gardiquimod showed greater antitumor potency compared to imiquimod.
Treatment activated NK cells, indicating an enhanced immune response.
Abstract
Background and Objectives: Toll-like receptors (TLRs) are pattern recognition receptors with an essential role in regulating both the innate and adaptive immune response. Given their pleiotropic effects in mounting an immune response, previous studies have proposed targeting these TLRs might render alternative strategies for cancer therapy. Synthetic immune response modifiers, such as imidazoquinolines, stimulate the immune cells by activating Toll-like receptors, particularly TLR7/8 receptors, consequently mounting an immune response. Agonists of this class activate, via TLR-mediated signaling, dendritic and B cells, as well as myeloid cells and T cells, thus exhibiting good prospects for cancer immunotherapy. In the present study, we sought to evaluate the effect of imiquimod and gardiquimod, two TLR 7 and 7/8 agonists, respectively, on tumor growth and phenotype of NK cells…
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Taxonomy
TopicsImmune Response and Inflammation · Immune Cell Function and Interaction · Immune cells in cancer
