TY - JOUR
T1 - Unleashing Natural IL18 Activity Using an Anti-IL18BP Blocker Induces Potent Immune Stimulation and Antitumor Effects
AU - Menachem, Assaf
AU - Alteber, Zoya
AU - Cojocaru, Gady
AU - Kfir, Tal Fridman
AU - Blat, Dan
AU - Leiderman, Olga
AU - Galperin, Moran
AU - Sever, Lital
AU - Cohen, Nadav
AU - Cohen, Keren
AU - Granit, Roy Z.
AU - Vols, Sandra
AU - Frenkel, Masha
AU - Soffer, Liron
AU - Meyer, Karin
AU - Menachem, Keren
AU - Tilleman, Hadas Galon
AU - Morein, Dina
AU - Borukhov, Itamar
AU - Toporik, Amir
AU - Shahor, Michal Perpinial
AU - Tatirovsky, Evgeny
AU - Mizrachi, Aviram
AU - Levy-Barda, Adva
AU - Sadot, Eran
AU - Strenov, Yulia
AU - Eitan, Ram
AU - Jakobson-Setton, Ariella
AU - Yanichkin, Natalia
AU - Ferre, Pierre
AU - Ophir, Eran
N1 - Publisher Copyright:
© 2024 The Authors.
PY - 2024/6/4
Y1 - 2024/6/4
N2 - Recombinant cytokines have limited anticancer efficacy mostly due to a narrow therapeutic window and systemic adverse effects. IL18 is an inflammasome-induced proinflammatory cytokine, which enhances T- and NK-cell activity and stimulates IFNγ production. The activity of IL18 is naturally blocked by a highaffinity endogenous binding protein (IL18BP). IL18BP is induced in the tumor microenvironment (TME) in response to IFNγ upregulation in a negative feedback mechanism. In this study, we found that IL18 is upregulated in the TME compared with the periphery across multiple human tumors and most of it is bound to IL18BP. Bound IL18 levels were largely above the amount required for T-cell activation in vitro, implying that releasing IL18 in the TME could lead to potent T-cell activation. To restore the activity of endogenous IL18, we generated COM503, a high-affinity anti-IL18BP that blocks the IL18BP:IL18 interaction and displaces precomplexed IL18, thereby enhancing T- and NK-cell activation. In vivo, administration of a surrogate anti-IL18BP, either alone or in combination with anti-PD-L1, resulted in significant tumor growth inhibition and increased survival across multiple mouse tumor models. Moreover, the anti-IL18BP induced pronounced TME-localized immune modulation including an increase in polyfunctional nonexhausted T- and NK-cell numbers and activation. In contrast, no increase in inflammatory cytokines and lymphocyte numbers or activation state was observed in serum and spleen. Taken together, blocking IL18BP using an Ab is a promising approach to harness cytokine biology for the treatment of cancer.
AB - Recombinant cytokines have limited anticancer efficacy mostly due to a narrow therapeutic window and systemic adverse effects. IL18 is an inflammasome-induced proinflammatory cytokine, which enhances T- and NK-cell activity and stimulates IFNγ production. The activity of IL18 is naturally blocked by a highaffinity endogenous binding protein (IL18BP). IL18BP is induced in the tumor microenvironment (TME) in response to IFNγ upregulation in a negative feedback mechanism. In this study, we found that IL18 is upregulated in the TME compared with the periphery across multiple human tumors and most of it is bound to IL18BP. Bound IL18 levels were largely above the amount required for T-cell activation in vitro, implying that releasing IL18 in the TME could lead to potent T-cell activation. To restore the activity of endogenous IL18, we generated COM503, a high-affinity anti-IL18BP that blocks the IL18BP:IL18 interaction and displaces precomplexed IL18, thereby enhancing T- and NK-cell activation. In vivo, administration of a surrogate anti-IL18BP, either alone or in combination with anti-PD-L1, resulted in significant tumor growth inhibition and increased survival across multiple mouse tumor models. Moreover, the anti-IL18BP induced pronounced TME-localized immune modulation including an increase in polyfunctional nonexhausted T- and NK-cell numbers and activation. In contrast, no increase in inflammatory cytokines and lymphocyte numbers or activation state was observed in serum and spleen. Taken together, blocking IL18BP using an Ab is a promising approach to harness cytokine biology for the treatment of cancer.
UR - http://www.scopus.com/inward/record.url?scp=85195229032&partnerID=8YFLogxK
U2 - 10.1158/2326-6066.CIR-23-0706
DO - 10.1158/2326-6066.CIR-23-0706
M3 - ???researchoutput.researchoutputtypes.contributiontojournal.article???
C2 - 38592331
AN - SCOPUS:85195229032
SN - 2326-6066
VL - 12
SP - 687
EP - 703
JO - Cancer immunology research
JF - Cancer immunology research
IS - 6
ER -