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IL-7–mediated expansion of autologous lymphocytes increases CD8+ VLA-4 expression and accumulation in glioblastoma models
Kirit Singh, … , Mustafa Khasraw, Peter E. Fecci
Kirit Singh, … , Mustafa Khasraw, Peter E. Fecci
Published April 17, 2025
Citation Information: J Clin Invest. 2025;135(12):e181471. https://doi.org/10.1172/JCI181471.
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Research Article Neuroscience Oncology

IL-7–mediated expansion of autologous lymphocytes increases CD8+ VLA-4 expression and accumulation in glioblastoma models

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Abstract

The efficacy of T cell–activating therapies against glioma is limited by an immunosuppressive tumor microenvironment and tumor-induced T cell sequestration. We investigated whether peripherally infused nonantigen specific autologous lymphocytes could accumulate in intracranial tumors. We observed that nonspecific autologous CD8+ ALT cells can indeed accumulate in this context, despite endogenous T cell sequestration in bone marrow. Rates of intratumoral accumulation were markedly increased when expanding lymphocytes with IL-7 compared with IL-2. Pretreatment with IL-7 ALT also enhanced the efficacy of multiple tumor-specific and nontumor-specific T cell–dependent immunotherapies against orthotopic murine and human xenograft gliomas. Mechanistically, we detected increased VLA-4 on mouse and human CD8+ T cells following IL-7 expansion, with increased transcription of genes associated with migratory integrin expression (CD9). We also observed that IL-7 increases S1PR1 transcription in human CD8+ T cells, which we have shown to be protective against tumor-induced T cell sequestration. These observations demonstrate that expansion with IL-7 enhances the capacity of ALT to accumulate within intracranial tumors and that pretreatment with IL-7 ALT can boost the efficacy of subsequent T cell–activating therapies against glioma. Our findings will inform the development of future clinical trials where ALT pretreatment can be combined with T cell–activating therapies.

Authors

Kirit Singh, Kelly M. Hotchkiss, Sarah L. Cook, Pamy Noldner, Ying Zhou, Eliese M. Moelker, Chelsea O. Railton, Emily E. Blandford, Bhairavy J. Puviindran, Shannon E. Wallace, Pamela K. Norberg, Gary E. Archer, Beth H. Shaz, Katayoun Ayasoufi, John H. Sampson, Mustafa Khasraw, Peter E. Fecci

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Figure 4

Expansion with IL-7 upregulates expression of the promigratory integrin VLA-4 on murine CD8+ T cells, which is required for enhanced intratumoral accumulation.

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Expansion with IL-7 upregulates expression of the promigratory integrin ...
(A) Representative gating strategy shown for VLA-4 expression on CD8+ T cells from IL-2 or IL-7 ALT. (B and C) CD8+ T cell VLA-4 expression (gMFI) and proportion of CD8+ VLA-4Hi T cells shown when expanding with IL-2 or IL-7 ALT (experiment outline in Figure 3, n = 4–6/group). (D and E) CD8+ T cell LFA-1 expression (gMFI) and proportion of CD8+ LFA-1Hi T cells shown when expanding with IL-2 or IL-7 ALT. (F and G) Analysis of the CD8+ T cell VLA-4Hi or LFA-1Hi proportion in ALT cellular product at expansion end (2 technical replicates). (H) Entry of CD45.1+CD8+ T cells in tumor following VLA-4Lo, VLA-4Hi ALT or VLA-4Hi ALT, and αVLA-4 (single-dose 200 μg intraperitoneal αVLA-4 antibody (BioXCell) pre-ALT, 3 pooled experiments shown, n = 8–20/group, 1-way ANOVA shown). (I) Evaluation of VLA-4 expression on the endogenous CD8+ T cell compartment over time (IL-2 and IL-7 treatment groups pooled, n = 9–12/group). Survival comparisons performed via log-rank (Mantel-Cox) χ2 test. Statistical analyses performed using unpaired t tests and data presented as mean ± SEM unless otherwise specified. *P < 0.05, **P ≤ 0.01, ***P < 0.001.

Copyright © 2025 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)

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