Enhanced glioblastoma immunotherapy via SMAC mimetic dose escalation and TGFβ blockade
Kyle Malone, Melanie Dugas, Nathalie Earl, Tommy Alain, Robert G Korneluk, Eric LaCasse, Shawn T Beug

TL;DR
This study explores how combining SMAC mimetic compounds with immune checkpoint inhibitors and TGFβ blockade can improve glioblastoma treatment in mice.
Contribution
The study identifies optimal dosing of SMAC mimetics and the added benefit of TGFβ blockade to enhance glioblastoma immunotherapy.
Findings
Increasing SMAC mimetic dose improves survival and reduces tumor-associated macrophages.
Combining SMAC mimetics with TGFβ blockade further enhances survival outcomes.
Central nervous system location limits anti-tumor immunity despite SMC and ICI treatment.
Abstract
Glioblastoma (GBM) is the most common primary brain tumor with an overall survival under 21 months. Despite extensive research effort, patient outcomes have improved minimally over the past several decades. The Inhibitor of Apoptosis (IAP) proteins are critical survival factors implicated in both immune regulation and gliomagenesis. Small molecule IAP antagonists called SMAC mimetic compounds (SMCs) are under investigation as cancer therapeutics across multiple malignancies, including GBM. SMCs induce GBM cell death in the presence of inflammatory cytokines, synergize with immune checkpoint inhibitors (ICI), and induce death of microglia and macrophages. Although SMCs show significant efficacy in murine models, complete eradication is not achieved. Here, we aimed to understand the limitations of SMCs in murine GBM and identify strategies to enhance efficacy of combination treatment with…
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Taxonomy
TopicsGlioma Diagnosis and Treatment · TGF-β signaling in diseases · Peptidase Inhibition and Analysis
