Antigen-IL-2 CAR-enhancer drives CAR-T fate and stemness, enhancing antitumor efficacy across models independent of IL-2Rα

Heydar Moravej; Taha Rakhshandehroo; Radia M M Khan; Victoria Marie Rivet; Elodie Marcandalli; Shreya R Mantri; Pegah Taklifi; Uk-Jae Lee; Benjamin B V Louis; Leila A Munaretto; Kathryn Regan; Zoe Farkash; Lea Berland; Zeina Gabr; Alexandra N Wolff; Antonia Kowalewski; Harris H Allen; Ali Nili; Jessika Baral; Dayna Mercadante; Mariateresa Fulciniti; Caron A Jacobson; Adam S Sperling; Omar Nadeem; Hadi T Nia; Michael Hemann; Nikhil C Munshi; Mohammad Rashidian

doi:10.1136/jitc-2025-013665

Antigen-IL-2 CAR-enhancer drives CAR-T fate and stemness, enhancing antitumor efficacy across models independent of IL-2Rα

J Immunother Cancer. 2026 Feb 18;14(2):e013665. doi: 10.1136/jitc-2025-013665.

Authors

Heydar Moravej^#¹, Taha Rakhshandehroo^#¹, Radia M M Khan^#¹, Victoria Marie Rivet^#¹, Elodie Marcandalli^#¹, Shreya R Mantri^#¹, Pegah Taklifi^#¹, Uk-Jae Lee^#¹, Benjamin B V Louis¹, Leila A Munaretto¹, Kathryn Regan², Zoe Farkash¹, Lea Berland¹, Zeina Gabr¹, Alexandra N Wolff^{1

3}, Antonia Kowalewski^{1

3}, Harris H Allen¹, Ali Nili¹, Jessika Baral^{1

3}, Dayna Mercadante^{4

5}, Mariateresa Fulciniti⁴, Caron A Jacobson^{3

4}, Adam S Sperling^{3

4

6}, Omar Nadeem^{3

4}, Hadi T Nia², Michael Hemann^{7

8}, Nikhil C Munshi^{3

4}, Mohammad Rashidian^{9

3

5

10}

Affiliations

¹ Department of Cancer Immunology and Virology, Dana-Farber Cancer Institute, Boston, Massachusetts, USA.
² Department of Biomedical Engineering, Boston University, Boston, Massachusetts, USA.
³ Harvard Medical School, Boston, Massachusetts, USA.
⁴ Department of Medical Oncology, Dana-Farber Cancer Insitute, Boston, Massachusetts, USA.
⁵ Parker Institute for Cancer Immunotherapy, San Francisco, California, USA.
⁶ Division of Hematology, Brigham and Women's Hospital, Boston, Massachusetts, USA.
⁷ David H. Koch Institute for Integrative Cancer Research, Cambridge, Massachusetts, USA.
⁸ Department of Biology, Massachusetts Institute of Technology, Cambridge, Massachusetts, USA.
⁹ Department of Cancer Immunology and Virology, Dana-Farber Cancer Institute, Boston, Massachusetts, USA mohammad_rashidian@dfci.harvard.edu.
¹⁰ Department of Radiology, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts, USA.

^# Contributed equally.

Abstract

Background: Limited durability of clinical responses remains a major challenge in chimeric antigen receptor (CAR)-T therapy. CAR-enhancers (CAR-Es), which fuse tumor antigens to interleukin (IL)-2 muteins, provide a targeted strategy to enhance CAR-T persistence and function. It remained unclear whether CAR-Es are effective across distinct tumor contexts, when using patient-derived T cells, or in preventing exhaustion and sustaining persistence. It was also unknown whether CAR-Es can selectively expand CAR-Ts in humanized mice with pre-existing T cells, and to what extent their efficacy depends on IL-2Rβγ vs IL-2Rα engagement. While IL-2Rα (CD25) has been classically linked to potent antitumor responses and memory formation, it also drives IL-2-associated toxicities, including vascular leak and preferential regulatory T cell expansion.

Methods: We systematically dissected CAR-E signaling requirements by engineering IL-2 variants with selective receptor affinities. Multiple CAR-E constructs were developed and tested across a range of in vitro and in vivo models.

Results: We demonstrate that CAR-E activity is entirely independent of IL-2Rα and critically dependent on IL-2Rβγ signaling. A next-generation IL-2Rα-sparing CAR-E maintained full potency, driving robust CAR-T expansion, persistence, and tumor clearance, even at low doses and when using CAR-T cells derived from previously treated multiple myeloma patients. These CAR-T cells not only resisted exhaustion but also re-expanded months later to eradicate tumor rechallenges. In humanized mice with pre-established T cells, CAR-Es selectively expanded CAR-Ts to dominate the circulating T-cell pool. CAR-E exerted a dominant influence on CAR-T fate, overriding tumor-derived cues and enforcing consistent phenotypes across diverse preclinical models.

Conclusions: These findings nominate a lead B-cell maturation antigen (BCMA)-IL-2 CAR-E candidate with strong translational potential for clinical development and establish IL-2Rβγ as a key driver of CAR-E activity. The results also identify IL-2Rα as dispensable and provide a mechanistic framework for designing safer, IL-2Rα-sparing CAR-Es.

Keywords: Chimeric antigen receptor - CAR; Cytokine; Multiple Myeloma.

MeSH terms

Animals
Antigens, Neoplasm* / immunology
Cell Line, Tumor
Humans
Immunotherapy, Adoptive* / methods
Interleukin-2 Receptor alpha Subunit* / metabolism
Interleukin-2* / genetics
Interleukin-2* / metabolism
Mice
Receptors, Chimeric Antigen* / genetics
Receptors, Chimeric Antigen* / immunology
Receptors, Chimeric Antigen* / metabolism
Xenograft Model Antitumor Assays

Substances

Interleukin-2
Receptors, Chimeric Antigen
Interleukin-2 Receptor alpha Subunit
Antigens, Neoplasm