Interleukin-2 signals converge in a lymphoid–dendritic cell pathway that promotes anticancer immunity

Raeber, Miro E.; Rosalia, Rodney Alexander; Schmid, Dominic; Karakus, Ufuk; Boyman, Onur

doi:10.1126/scitranslmed.aba5464

Cited by 61 publications

(58 citation statements)

References 74 publications

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“…A Tγδ17-MDSC immunosuppressive axis had been previously identified in human colorectal carcinoma, 43 which could be disrupted by IL-2c treatment based on our data. Further, RAG1 KO mice have functional innate lymphoid cells that contributed to IL-2c efficacy against subcutaneous B16 melanoma challenge, 12 whereas IL-2c did not treat subcutaneous MB49 in these studies, further supporting tissue- and/or tumor-specific IL-2c effects requiring additional investigations.…”

Section: Discussionmentioning

confidence: 76%

“… 43 Interestingly, we found that IL-2c reduced the frequency ( figure 6D ) and number ( figure 6E ) of bladder TNF-α + Vγ4δ4 cells, with a concomitant reduction in PMN-MDSC frequency ( figure 6F ). Intratumoral monocytic MDSC (M-MDSC) content was unchanged by IL-2c ( online supplemental figure S4E ), suggesting that IL-2c treatment could include a specific reduction of PMN-MDSCs, possibly via IL-17 or TNF-α effects that could include IL-2c-induced TNF-α production by innate lymphoid cells recently described in a subcutaneous melanoma model, 12 an area requiring further investigation.…”

Section: Resultsmentioning

confidence: 93%

“… 53 We found that IL-2c reduced orthotopic PMN-MDSC frequency, which could be from an IL-17/TNF-α signaling effect based on prior reports, 43 and could specifically include TNF-α from innate lymphoid cells, a novel IL-2c effect just reported. 12 MDSC-mediated immunosuppression of BC immunotherapy responses merit additional investigation and may be linked to other beneficial IL-2c effects. A Tγδ17-MDSC immunosuppressive axis had been previously identified in human colorectal carcinoma, 43 which could be disrupted by IL-2c treatment based on our data.…”

Section: Discussionmentioning

confidence: 99%

“… 9 10 CD122-directed IL-2 therapy using distinct molecules is also promising in human BC trials, including when combined with αPD-1. 11 Effects on other CD25 + and CD122 + cells including γδ T cells using targeted IL-2 therapies are unreported to our knowledge and recent reports suggest IL-2c can also act through non-IL-2 receptor expressing cells such as dendritic cells, 12 necessitating improved understanding of specific treatment mechanisms in distinct tumor microenvironments.…”

Section: Introductionmentioning

confidence: 99%

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CD122-directed interleukin-2 treatment mechanisms in bladder cancer differ from αPD-L1 and include tissue-selective γδ T cell activation

Reyes

Deng

Zhang

et al. 2021

J Immunother Cancer

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BackgroundAnti-programmed death-ligand 1 (αPD-L1) immunotherapy is approved to treat bladder cancer (BC) but is effective in <30% of patients. Interleukin (IL)-2/αIL-2 complexes (IL-2c) that preferentially target IL-2 receptor β (CD122) augment CD8+ antitumor T cells known to improve αPD-L1 efficacy. We hypothesized that the tumor microenvironment, including local immune cells in primary versus metastatic BC, differentially affects immunotherapy responses and that IL-2c effects could differ from, and thus complement αPD-L1.MethodsWe studied mechanisms of IL-2c and αPD-L1 efficacy using PD-L1+ mouse BC cell lines MB49 and MBT-2 in orthotopic (bladder) and metastatic (lung) sites.ResultsIL-2c reduced orthotopic tumor burden and extended survival in MB49 and MBT-2 BC models, similar to αPD-L1. Using antibody-mediated cell depletions and genetically T cell-deficient mice, we unexpectedly found that CD8+ T cells were not necessary for IL-2c efficacy against tumors in bladder, whereas γδ T cells, not reported to contribute to αPD-L1 efficacy, were indispensable for IL-2c efficacy there. αPD-L1 responsiveness in bladder required conventional T cells as expected, but not γδ T cells, altogether defining distinct mechanisms for IL-2c and αPD-L1 efficacy. γδ T cells did not improve IL-2c treatment of subcutaneously challenged BC or orthotopic (peritoneal) ovarian cancer, consistent with tissue-specific and/or tumor-specific γδ T cell contributions to IL-2c efficacy. IL-2c significantly altered bladder intratumoral γδ T cell content, activation status, and specific γδ T cell subsets with antitumor or protumor effector functions. Neither IL-2c nor αPD-L1 alone treated lung metastatic MB49 or MBT-2 BC, but their combination improved survival in both models. Combination treatment efficacy in lungs required CD8+ T cells but not γδ T cells.ConclusionsMechanistic insights into differential IL-2c and αPD-L1 treatment and tissue-dependent effects could help develop rational combination treatment strategies to improve treatment efficacy in distinct cancers. These studies also provide insights into γδ T cell contributions to immunotherapy in bladder and engagement of adaptive immunity by IL-2c plus αPD-L1 to treat refractory lung metastases.

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Section: Discussionmentioning

confidence: 76%

Section: Resultsmentioning

confidence: 93%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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CD122-directed interleukin-2 treatment mechanisms in bladder cancer differ from αPD-L1 and include tissue-selective γδ T cell activation

Reyes

Deng

Zhang

et al. 2021

J Immunother Cancer

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“…Furthermore, accumulated evidence suggests that IL2 signaling in the TME favors responsiveness to PD1 blockade. [70][71][72][73] As shown in figure 7H,I, skin immunization resulted in the recruitment of increased levels of IL2 + CD4 + TIL in the tumor core, which may at least partially explain the ability of skin immunization to convert PD1-resistant tumors into αPD1responsive tumors (figures 2A and 4D).…”

Section: Skin Immunization Improves Therapeutic Efficacy Over DC Cellmentioning

confidence: 99%

Skin immunization for effective treatment of multifocal melanoma refractory to PD1 blockade and Braf inhibitors

Hao

Falo²,

Chen

et al. 2021

J Immunother Cancer

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BackgroundDespite the remarkable benefits associated with the interventional treatment of melanomas (and other solid cancers) with immune checkpoint and Braf inhibitors (Brafi), most patients ultimately progress on therapy. The presence of multifocal/disseminated disease in patients increases their mortality risk. Hence, the development of novel strategies to effectively treat patients with melanomas that are resistant to anti-PD1 mAb (αPD1) and/or Brafi, particularly those with multifocal/disseminated disease remains a major unmet clinical need.MethodsMice developing induced/spontaneous BrafV600E/Pten−/− melanomas were treated by cutaneous immunization with a DNA vaccine encoding the melanoma-associated antigen TRP2, with Brafi or αPD1 alone, or with a combination of these treatments. Tumor progression, tumor-infiltration by CD4+ and CD8+ T cells, and the development of TRP2-specific CD8+ T cells were then monitored over time.ResultsVaccination led to durable antitumor immunity against PD1/Brafi-resistant melanomas in both single lesion and multifocal disease models, and it sensitized PD1-resistant melanomas to salvage therapy with αPD1. The therapeutic efficacy of the vaccine was associated with host skin-resident cells, the induction of a systemic, broadly reactive IFNγ+CD8+ T cell repertoire, increased frequencies of CD8+ TIL and reduced levels of PD1hi/intCD8+ T cells. Extended survival was associated with improved TIL functionality, exemplified by the presence of enhanced levels of IFNγ+CD8+ TIL and IL2+CD4+ TIL.ConclusionsThese data support the use of a novel genetic vaccine for the effective treatment of localized or multifocal melanoma refractory to conventional αPD1-based and/or Brafi-based (immune)therapy.

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IL-2 promotes expansion and intratumoral accumulation of tumor infiltrating dendritic cells in pancreatic cancer

Gong,

Huang,

Wang

et al. 2024

Cancer Immunol Immunother

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This study aims to investigate the diagnostic potential of IL-2 for PDAC and develop a method to improve the dendritic cell (DC) based vaccine against PDAC. The gene expression data and clinical characteristics information for 178 patients with PDAC were obtained from The Cancer Genome Atlas (TCGA). DCs were isolated from Human peripheral blood mononuclear cells (PBMCs) and were cultured in 4 different conditions. DCs were pulsed by tumor cell lysates or KRAS G12D1 − 23 peptide, and then used to activate T cells. The mixture of DCs and T cells were administered to xenograft mouse model through the tail vein. The infiltration of DCs and T cells were detected by immunohistochemistry. The generation of KRAS G12D mutation specific cytotoxic T cells was determined by in vitro killing assay. We observed that PDAC patients with higher IL-2 mRNA levels exhibited improved overall survival and increased infiltration of CD8 + T cells, NK cells, naïve B cells, and resting myeloid DCs in the tumor microenvironment. IL-2 alone did not enhance DC proliferation, antigen uptake, or apoptosis inhibition unless co-cultured with PBMCs. DCs co-cultured with PBMCs in IL-2-containing medium demonstrated the strongest tumor repression effect in vitro and in vivo. Compared to DCs obtained through the traditional method (cultured in medium containing GM-CSF and IL-4), DCs cultured with PBMCs, and IL-2 exhibited increased tumor infiltration capacity, potentially facilitating sustained T cell immunity. DCs cultured in the PBMCs-IL-2 condition could promote the generation of cytotoxic T cells targeting tumor cells carrying KRAS G12D mutation.

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Interleukin-2 signals converge in a lymphoid–dendritic cell pathway that promotes anticancer immunity

Cited by 61 publications

References 74 publications

CD122-directed interleukin-2 treatment mechanisms in bladder cancer differ from αPD-L1 and include tissue-selective γδ T cell activation

CD122-directed interleukin-2 treatment mechanisms in bladder cancer differ from αPD-L1 and include tissue-selective γδ T cell activation

Skin immunization for effective treatment of multifocal melanoma refractory to PD1 blockade and Braf inhibitors

IL-2 promotes expansion and intratumoral accumulation of tumor infiltrating dendritic cells in pancreatic cancer

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