Conventional type I dendritic cells maintain a reservoir of proliferative tumor-antigen specific TCF-1+ CD8+ T cells in tumor-draining lymph nodes

Schenkel, Jason M.; Herbst, Rebecca H.; Canner, David; Li, Amy; Hillman, Michelle; Shanahan, Sean-Luc; Gibbons, Grace; Smith, Olivia; Kim, Jonathan Y.; Westcott, Peter M.K.; Hwang, William L.; Freed-Pastor, William A.; Eng, George; Cuoco, Michael S.; Rogers, Patricia; Park, Jin K.; Burger, M.; Rozenblatt-Rosen, Orit; Cong, Le; Pauken, Kristen E.; Regev, Aviv; Jacks, Tyler

doi:10.1016/j.immuni.2021.08.026

Cited by 151 publications

(120 citation statements)

References 60 publications

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“…One possible explanation for our results would be enhanced migration of antigen-loaded CD103 + cDC1s into the draining lymph nodes, potentially resulting in expansion of the antigen-specific TCF1 + stem-like population of CD8 + T cells that are necessary to maintain an immune response within tumors. 14 15 This could also be CXCR3 dependent, as CXCL9 expression by myeloid cells within the lymph nodes is important for memory responses to viral infections. 16 To evaluate this, we made use of a PyMT tumor cell line expressing the pH-insensitive fluorophore ZsGreen (PyMT-ZsGreen).…”

Section: Resultsmentioning

confidence: 99%

TIM-3 blockade enhances IL-12-dependent antitumor immunity by promoting CD8⁺T cell and XCR1⁺dendritic cell spatial co-localization

Gardner

Pulido

Hänggi

et al. 2022

J Immunother Cancer

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BackgroundT cell immunoglobulin and mucin domain containing−3 (TIM-3) blocking antibodies are currently being evaluated in clinical trials for solid and hematological malignancies. Despite its identification on T cells, TIM-3 is predominantly expressed by myeloid cells, including XCR1+ type I conventional dendritic cells (cDC1s). We have recently shown that TIM-3 blockade promotes expression of CXCR3 chemokine ligands by tumor cDCs, but how this drives a CD8+ T cell-dependent response to therapy is unclear.MethodsT cell infiltration, effector function, and spatial localization in relation to XCR1+ cDC1s were evaluated in a murine orthotopic mammary carcinoma model during response to TIM-3 blockade and paclitaxel chemotherapy. Mixed bone marrow chimeras and diphtheria toxin depletion were used to determine the role of specific genes in cDC1s during therapeutic responses.ResultsTIM-3 blockade increased interferon-γ expression by CD8+ T cells without altering immune infiltration. cDC1 expression of CXCL9, but not CXCL10, was required for response to TIM-3 blockade. CXCL9 was also necessary for the increased proximity observed between CD8+ T cells and XCR1+ cDC1s during therapy. Tumor responses were dependent on cDC1 expression of interleukin-12, but not MHCI.ConclusionsTIM-3 blockade increases exposure of intratumoral CD8+ T cells to cDC1-derived cytokines, with implications for the design of therapeutic strategies using antibodies against TIM-3.

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Section: Resultsmentioning

confidence: 99%

TIM-3 blockade enhances IL-12-dependent antitumor immunity by promoting CD8⁺T cell and XCR1⁺dendritic cell spatial co-localization

Gardner

Pulido

Hänggi

et al. 2022

J Immunother Cancer

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“…The importance of the TDLN in mediating a robust, RT-stimulated, anti-tumor response and RT s synergy with ICI has recently been reported, but only begun to be characterized [67,68]. The TDLN plays a critical role in T cell stimulation through activating DCs and concentrating tumor antigens [67,69,70]. Furthermore, there appears to be a progenitor sub-population of CD8 + T cells both within the tumor and TDLN that is critical for robust PD-1 therapy responses [71,72].…”

Section: Pre-clinical Datamentioning

confidence: 99%

The Abscopal Effect: A Review of Pre-Clinical and Clinical Advances

Janopaul‐Naylor

Shen

Qian

et al. 2021

IJMS

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Radiotherapy has been used for more than a hundred years to cure or locally control tumors. Regression of tumors outside of the irradiated field was occasionally observed and is known as the abscopal effect. However, the occurrence of systemic anti-tumor effects was deemed too rare and unpredictable to be a therapeutic goal. Recent studies suggest that immunotherapy and radiation in combination may enhance the abscopal response. Increasing numbers of cases are being reported since the routine implementation of immune checkpoint inhibitors, showing that combined radiotherapy with immunotherapy has a synergistic effect on both local and distant (i.e., unirradiated) tumors. In this review, we summarize pre-clinical and clinical reports, with a specific focus on the mechanisms behind the immunostimulatory effects of radiation and how this is enhanced by immunotherapy.

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“…Nevertheless, our data suggests that cDC-1s may have an inherent capacity to promote memory fate, which may contribute to the T MEM niche. In support of this proposed function, recent evidence demonstrated that cDC-1s are critical for maintaining a reservoir of stem-like cells in tumor-draining lymph nodes (Schenkel et al 2021). It is interesting to note that cDC-1s can bias CD4+ T cells towards the T REG lineage, which can be potent sources of TGF-b, whereas cDC-2s tend to induce an effector T helper 1 (T H1 ) fate (Brown et al, 2019;Opejin et al, 2020).…”

Section: Discussionmentioning

confidence: 92%

CXCR3 regulates stem and proliferative CD8+ T cells during chronic infection by promoting interactions with DCs in splenic bridging channels

et al. 2022

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Conventional type I dendritic cells maintain a reservoir of proliferative tumor-antigen specific TCF-1+ CD8+ T cells in tumor-draining lymph nodes

Cited by 151 publications

References 60 publications

TIM-3 blockade enhances IL-12-dependent antitumor immunity by promoting CD8⁺T cell and XCR1⁺dendritic cell spatial co-localization

TIM-3 blockade enhances IL-12-dependent antitumor immunity by promoting CD8⁺T cell and XCR1⁺dendritic cell spatial co-localization

The Abscopal Effect: A Review of Pre-Clinical and Clinical Advances

CXCR3 regulates stem and proliferative CD8+ T cells during chronic infection by promoting interactions with DCs in splenic bridging channels

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Conventional type I dendritic cells maintain a reservoir of proliferative tumor-antigen specific TCF-1+ CD8+ T cells in tumor-draining lymph nodes

Cited by 151 publications

References 60 publications

TIM-3 blockade enhances IL-12-dependent antitumor immunity by promoting CD8+T cell and XCR1+dendritic cell spatial co-localization

TIM-3 blockade enhances IL-12-dependent antitumor immunity by promoting CD8+T cell and XCR1+dendritic cell spatial co-localization

The Abscopal Effect: A Review of Pre-Clinical and Clinical Advances

CXCR3 regulates stem and proliferative CD8+ T cells during chronic infection by promoting interactions with DCs in splenic bridging channels

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Product

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TIM-3 blockade enhances IL-12-dependent antitumor immunity by promoting CD8⁺T cell and XCR1⁺dendritic cell spatial co-localization

TIM-3 blockade enhances IL-12-dependent antitumor immunity by promoting CD8⁺T cell and XCR1⁺dendritic cell spatial co-localization