PD1-IL2v expands and induces effector CD8+ TILs, but not Tregs, in the BCG treated orthotopic non-muscle invasive bladder cancer model
Irene Locatelli, Marco Lorenzoni, Chiara Venegoni, Alessia Di Coste, Rita Sorrentino, Jithin Jose, Daniela Maria Cirillo, Patrick Weber, Amrita Manchala, Ralf J. Hosse, Valeria Nicolini, Pablo Umana, Christian Klein, Andrea Salonia, Francesco Montorsi, Matteo Bellone

TL;DR
A new treatment combining BCG with PD1-IL2v boosts CD8+ T cells in bladder cancer without increasing harmful Tregs, potentially improving patient outcomes.
Contribution
The study introduces a targeted therapy combining BCG with PD1-IL2v to selectively enhance CD8+ TILs while avoiding Treg expansion in bladder cancer.
Findings
The combination of BCG and PD1-IL2v significantly increased cytotoxic CD8+ TILs with a polyfunctional effector phenotype.
The treatment avoided Treg expansion, unlike BCG monotherapy.
Patient-derived tumors showed a higher frequency of CD8+ TILs compared to Tregs, with many CD8+ TILs expressing PD-1.
Abstract
The combination of systemic immune checkpoint inhibitors with standard of care intravesical Bacillus Calmette-Guerin (BCG) therapy for non-muscle invasive bladder cancer (NMIBC) has shown potential in enhancing BCG therapeutic effects. However, challenges such as disease recurrence, progression, and immune-related toxicities remain a significant hurdle. Furthermore, the mechanism of action of BCG involves broad, non-specific immune activation. While this recruits bystander CD8+ and NK cells, it also triggers the undesired expansion of Tregs, which may ultimately hamper therapeutic efficacy. We aimed to explore the feasibility of a targeted approach designed to overcome intravesical tumor resistance and selectively enhance the expansion and effector functions of CD8+ TILs. We tested intravesical administration of BCG with murinized PD1-IL2v, a fusion protein that simultaneously targets…
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Taxonomy
TopicsBladder and Urothelial Cancer Treatments · Immune responses and vaccinations · Cancer Immunotherapy and Biomarkers
