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Development of DPP-4-resistant CXCL9-Fc and CXCL10-Fc chemokines for effective cancer immunotherapy

Jennie Lugassy, Noor Abdala-Saleh, Ghada Jarrous, Abeer Turky, Daniel Saidemberg, Gabriela Ridner-Bahar, Nir Berger, Dana Bar-On, Tetsuya Taura, David S. Wilson, Nathan Karin

2025Proceedings of the National Academy of Sciences14 citationsDOIOpen Access PDF

Abstract

CXCR3 is a chemokine receptor for three ligands: CXCL9, CXCL10, and CXCL11. Accumulating evidence, including data presented here, suggests that the interaction between CXCL9/CXCL10 and CXCR3 not only attracts CXCR3+ T cells but also promotes the induction of IFNγ- high effector/cytotoxic CD4+ and CD8+ T cells, establishing a CXCL9/10-CXCR3-IFNγ self-amplifying cycle that promotes efficient cancer cell killing. One of the homeostatic mechanisms that may limit this cycle is the cleavage of the two N-terminal amino acids of these chemokines by Dipeptidyl Peptidase IV (DPP-4). The modified chemokines retain their ability to bind CXCR3 but no longer activate it, becoming competitive antagonists to native CXCL9/CXCL10. To develop a DPP-4-resistant variant, we combined biochemical analysis with computational modeling, demonstrating that the addition of N-terminal glutamine (Q) to CXCL9-Fc and CXCL10-Fc rendered them fully active CXCR3 agonists, yet resistant to DPP-4 cleavage. Preclinical evaluations imply that they offer significant therapeutic potential in cancer immunotherapy.

Topics & Concepts

CXCL9CXCR3CXCL10CXCL11Cancer immunotherapyChemokineChemokine receptorCancer researchCXCL14ChemistryBiologyImmunotherapyCell biologyReceptorImmunologyBiochemistryImmune systemPeptidase Inhibition and AnalysisChemokine receptors and signalingImmunotherapy and Immune Responses
Development of DPP-4-resistant CXCL9-Fc and CXCL10-Fc chemokines for effective cancer immunotherapy | Litcius