Blockade of immune checkpoints in lymph nodes through locoregional delivery augments cancer immunotherapy

Francis, David M.; Manspeaker, Margaret P.; Schudel, Alex; Sestito, Lauren F.; O’Melia, Meghan J.; Kissick, Haydn; Pollack, Brian P.; Waller, Edmund K.; Thomas, Susan N.

doi:10.1126/scitranslmed.aay3575

Cited by 151 publications

(139 citation statements)

References 52 publications

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“…We reported that peritumoral delivery of anti-CTLA-4 in mouse models resulted in an equally efficient antitumor response as observed after systemic administration, without the usually associated inflammatory side effects (65). A recent report from Francis et al (6) elegantly showed in tumor models that intratumoral administration of CTLA-4 and/or PD-1 blocking antibodies ensured optimal access to TDLN (in contrast to systemic administration) and, moreover, that ipsilateral administration on a site different from the tumor but with lymph drainage to the same lymph node stations afforded equal tumor protection. This is in line with our own observations of the induction of systemic and protective antimelanoma immunity in early-stage melanoma through local immune modulation of the SLN after surgical removal of the primary tumor, either by CpG-B (44) or by anti-CTLA-4 (71).…”

Section: In Conclusion: the Rise Of Local Immunotherapymentioning

confidence: 74%

“…Such earlyeffector or progenitor-exhausted T cells can persist for long times in the TDLN in the absence of antigen, are polyfunctional, display a high proliferative capacity and share phenotypic traits with central-memory T cells (58). Upon PD-1 blockade they can efficiently home to the TME and there expand further and differentiate into effector T cells (6,26). In keeping with this, Chow et al showed that expression of CXCR3, required for tumor rejection after PD-1 blockade in the MC38 mouse model, was expressed at high levels by progenitor-exhausted or early-effector T cells, whereas it was hardly expressed by terminally exhausted T cells (59).…”

Section: Overcoming Immune Exclusion By Targeting DC In Tdln: Reinvigmentioning

confidence: 99%

“…An intense research effort has therefore been ongoing to characterize the tumor microenvironment (TME) and find ways to ensure T-cell infiltration (3,4). New insights point to the need for therapeutic targeting of tumor-draining lymph nodes (TDLN), rather than of the TME, to secure proper antitumor T-cell generation and at the same time brisk tumor infiltration (5)(6)(7)(8). TDLN can either be more proximal or more distal from the tumor, but they are all part of the lymph catchment area of the tumor.…”

Section: Introductionmentioning

confidence: 99%

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Immunotherapy Goes Local: The Central Role of Lymph Nodes in Driving Tumor Infiltration and Efficacy

et al. 2021

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Immune checkpoint blockade (ICB) has changed the therapeutic landscape of oncology but its impact is limited by primary or secondary resistance. ICB resistance has been related to a lack of T cells infiltrating into the tumor. Strategies to overcome this hurdle have so far focused on the tumor microenvironment, but have mostly overlooked the role of tumor-draining lymph nodes (TDLN). Whereas for CTLA-4 blockade TDLN have long since been implicated due to its perceived mechanism-of-action involving T cell priming, only recently has evidence been emerging showing TDLN to be vital for the efficacy of PD-1 blockade as well. TDLN are targeted by developing tumors to create an immune suppressed pre-metastatic niche which can lead to priming of dysfunctional antitumor T cells. In this review, we will discuss the evidence that therapeutic targeting of TDLN may ensure sufficient antitumor T cell activation and subsequent tumor infiltration to facilitate effective ICB. Indeed, waves of tumor-specific, proliferating stem cell-like, or progenitor exhausted T cells, either newly primed or reinvigorated in TDLN, are vital for PD-1 blockade efficacy. Both tumor-derived migratory dendritic cell (DC) subsets and DC subsets residing in TDLN, and an interplay between them, have been implicated in the induction of these T cells, their imprinting for homing and subsequent tumor control. We propose that therapeutic approaches, involving local delivery of immune modulatory agents for optimal access to TDLN, aimed at overcoming hampered DC activation, will enable ICB by promoting T cell recruitment to the tumor, both in early and in advanced stages of cancer.

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Section: In Conclusion: the Rise Of Local Immunotherapymentioning

confidence: 74%

Section: Overcoming Immune Exclusion By Targeting DC In Tdln: Reinvigmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Immunotherapy Goes Local: The Central Role of Lymph Nodes in Driving Tumor Infiltration and Efficacy

et al. 2021

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“…Accumulating results were reported by recent clinical trials involving cancer immunotherapy with various immune checkpoint inhibitors (ICIs)—including antibodies against cytotoxic T-lymphocyte-associated protein 4 (CTLA-4) and monoclonal antibodies (mAbs) against both programmed cell death-1 and the dysfunction/activation of cytotoxic T lymphocytes [ 1 , 2 , 3 , 4 , 5 , 6 , 7 , 8 ]. The blockade of immune checkpoints by ICIs reinvigorates dysfunctional T cells by restoring tumor-specific immunity for the eradication of cancer cells.…”

Section: Introductionmentioning

confidence: 99%

Targeting the Tumor Microenvironment for Improving Therapeutic Effectiveness in Cancer Immunotherapy: Focusing on Immune Checkpoint Inhibitors and Combination Therapies

Chyuan

Chu

Hsu

2021

Cancers

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Immune checkpoints play critical roles in the regulation of T-cell effector function, and the effectiveness of their inhibitors in cancer therapy has been established. Immune checkpoint inhibitors (ICIs) constitute a paradigm shift in cancer therapy in general and cancer immunotherapy in particular. Immunotherapy has been indicated to reinvigorate antitumor T-cell activity and dynamically modulate anticancer immune responses. However, despite the promising results in the use of immunotherapy in some cancers, numerous patients do not respond to ICIs without the existence of a clear predictive biomarker. Overall, immunotherapy involves a certain degree of uncertainty and complexity. Research on the exploration of cellular and molecular factors within the tumor microenvironment (TME) aims to identify possible mechanisms of immunotherapy resistance, as well as to develop novel combination strategies involving the specific targeting of the TME for cancer immunotherapy. The combination of this approach with other types of treatment, including immune checkpoint blockade therapy involving multiple agents, most of the responses and effects in cancer therapy could be significantly enhanced, but the appropriate combinations have yet to be established. Moreover, the in-depth exploration of complexity within the TME allows for the exploration of pathways of immune dysfunction. It may also aid in the identification of new therapeutic targets. This paper reviews recent advances in the improvement of therapeutic efficacy on the immune context of the TME and highlights its contribution to cancer immunotherapy.

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“…Further studies will be needed to test what signals are necessary for maintenance and migration of T cells in dLNs.The role of the dLN in immunotherapy remains uncertain. Expression of PD-L1on DCs is important for responses to anti-PD-L1 in some tumor models, and migratory DCs in tumor dLNs express both PD-L1 and the costimulatory receptor B7-2 (98).Moreover, PD-1 blockade can act in dLNs in transplant tumor models(99,100).Whether PD-1 blockade acts outside the TME in humans is not known, but therapeutic efficacy after anti-PD-1 treatment in patients is associated with changes in immune cell populations in the peripheral blood(101,102) and with the appearance of new T cell clones in the tumor after therapy(103)(104)(105). Our analyses of CD8 T cells from humans showed the presence of TSL-like cells in LNs and tumors.…”

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confidence: 99%

A reservoir of stem-like CD8 T cells in the tumor-draining lymph node maintains the ongoing anti-tumor immune response

Connolly

Kuchroo

Venkat

et al. 2021

Preprint

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Abstract“Stem-like” TCF1+ CD8+ T cells (TSL) are necessary for long-term maintenance of T cell responses and the efficacy of immunotherapy but, as tumors contain signals that should drive T-cell terminal-differentiation, how these cells are maintained in tumors remains unclear. We found that a small number of TCF1+ tumor-specific CD8+ T cells were present in tumors throughout development. Yet, most intratumoral T cells differentiated as tumors progressed, corresponding with an immunologic shift in the tumor microenvironment (TME) from “hot” to “cold”. By contrast, most tumor-specific CD8+ T cells in tumor-draining lymph nodes (dLNs) had functions and gene expression signatures similar to TSL from chronic LCMV infection and this population was stable over time, despite the changes in the TME. dLN T cells were the precursors of their more-differentiated intratumoral counterparts, and maintenance of TCF1 by intratumoral T cells required continuous migration from dLNs. Finally, TSL CD8 T cells were also present in LNs from lung adenocarcinoma patients, suggesting this population is also relevant in human disease. Thus, we propose that the dLN TSL reservoir has a critical function during tumor development in sustaining antitumor T cells during tumor development and protecting them from the terminal differentiation that occurs in the TME.

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Blockade of immune checkpoints in lymph nodes through locoregional delivery augments cancer immunotherapy

Cited by 151 publications

References 52 publications

Immunotherapy Goes Local: The Central Role of Lymph Nodes in Driving Tumor Infiltration and Efficacy

Immunotherapy Goes Local: The Central Role of Lymph Nodes in Driving Tumor Infiltration and Efficacy

Targeting the Tumor Microenvironment for Improving Therapeutic Effectiveness in Cancer Immunotherapy: Focusing on Immune Checkpoint Inhibitors and Combination Therapies

A reservoir of stem-like CD8 T cells in the tumor-draining lymph node maintains the ongoing anti-tumor immune response

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