L-DOS47 enhances response to immunotherapy in pancreatic cancer tumor

Bruna V. Jardim‐Perassi(Moffitt Cancer Center), Pietro Irrera(Moffitt Cancer Center), Dominique Abrahams(University of South Florida), Verónica Estrella(Moffitt Cancer Center), Bryce Ordway(Harvard University), Samantha Byrne(Moffitt Cancer Center), Andrew A. Ojeda(Moffitt Cancer Center), Christopher J. Whelan(Moffitt Cancer Center), Jongphil Kim(Moffitt Cancer Center), Matthew Beatty(Moffitt Cancer Center), Sultan Damgaci-Erturk(United States Military Academy), Dario Livio Longo(Institute of Biostructure and Bioimaging), Kim Gaspar(Helix Biopharma (Canada)), Gabrielle M. Siegers(Helix Biopharma (Canada)), Barbara A. Centeno(Moffitt Cancer Center), Justin Y. C. Lau(Moffitt Cancer Center), Arig Ibrahim-Hashim(Moffitt Cancer Center), Shari Pilon‐Thomas(Moffitt Cancer Center), Robert J. Gillies(Moffitt Cancer Center)
bioRxiv (Cold Spring Harbor Laboratory)
August 28, 2023
10.1101/2023.08.28.555194
Cited by 0Open Access
Full Text

Abstract

Acidosis is an important immunosuppressive mechanism that leads to tumor growth. Therefore, we investigated the neutralization of tumor acidity to improve immunotherapy response. L-DOS47, a new targeted urease immunoconjugate designed to neutralize tumor acidity, has been well tolerated in phase I/IIa trials. L-DOS47 binds CEACAM6, a cell surface protein highly expressed in gastrointestinal cancers, allowing urease to cleave endogenous urea into two NH4+ and one CO2, thereby raising local pH. To test the synergetic effect of neutralizing tumor acidity with immunotherapy, we developed a pancreatic orthotopic murine tumor model (KPC961) expressing human CEACAM6. Our results demonstrate that combining L DOS47 with anti-PD1 significantly increases the efficacy of anti-PD1 monotherapy, reducing tumor growth for up to 4 weeks.

Related Papers

No related papers found

Powered by citation graph analysis