IL-2/CD40-activated macrophages rescue age and tumor-induced T cell dysfunction in elderly mice

Jackaman, Connie; Dye, Danielle E.; Nelson, Delia J.

doi:10.1007/s11357-014-9655-y

Cited by 24 publications

(17 citation statements)

References 46 publications

(72 reference statements)

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“…We have previously shown that intra-tumoral IL-2 combined with anti-CD40 antibody leads to AE17 mesothelioma tumor regression in young mice; this was associated with increased CTL activity ( Jackaman et al, 2008 , 2016 ). Furthermore, in vitro studies showed that elderly derived IL-2/anti-CD40-activated macrophages could restore age- and tumor-related T cell function ( Jackaman et al, 2013 , 2014 ). Therefore, we next examined whether IL-2/anti-CD40 was effective in young vs. elderly AE17 tumor-bearing mice and whether macrophages contributed to the efficacy of IL-2/anti-CD40 immunotherapy.…”

Section: Resultsmentioning

confidence: 99%

“…This response included the generation of anti-tumor CTLs and polarization of macrophages into a pro-inflammatory phenotype within DLNs in young mice in vivo ( Jackaman et al, 2016 ). Similarly, we have shown that IL-2/anti-CD40-activated macrophages can rescue age- and tumor-induced T cell function in vitro ( Jackaman et al, 2013 , 2014 ). However, it is likely that the inflammaging microenvironment plays a pivotal role in age-related macrophage dysfunction ( Oishi and Manabe, 2016 ) and further in vivo studies are required.…”

Section: Introductionmentioning

confidence: 81%

“…However, in separate studies BM-derived macrophages from elderly female C57BL/6J mice (aged 16–22 months) exhibited increased TNF-α and IL-6 production in response to LPS ( Bouchlaka et al, 2013 ; Thevaranjan et al, 2017 ). Similarly, elderly derived female Balb/c (aged 17–18 months) and C57BL/6J peritoneal macrophages (aged 24–28 months) displayed hypersensitivity to anti-inflammatory IL-4 stimuli with increased production of anti-inflammatory IL-10 and TGF-β ( Jackaman et al, 2013 , 2014 ). In vivo murine studies have also described macrophages from the eye, muscles, lymph nodes, spleen and bone marrow expressing increased IL-10 during aging ( Wang et al, 1995 , 2015 ; Kelly et al, 2007 ; Jackaman et al, 2013 ).…”

Section: Introductionmentioning

confidence: 99%

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Macrophage Depletion in Elderly Mice Improves Response to Tumor Immunotherapy, Increases Anti-tumor T Cell Activity and Reduces Treatment-Induced Cachexia

et al. 2018

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Most cancers emerge in the elderly, including lung cancer and mesothelioma, yet the elderly remain an underrepresented population in pre-clinical cancer studies and clinical trials. The immune system plays a critical role in the effectiveness of many anti-cancer therapies in young hosts via tumor-specific T cells. However, immunosuppressive macrophages can constitute up to 50% of the tumor burden and impair anti-tumor T cell activity. Altered macrophage phenotype and function during aging may further impact anti-tumor T cell responses. Yet, the impact of macrophages on anti-tumor T cell responses and immunotherapy in the elderly is unknown. Therefore, we examined macrophages and their interaction with T cells in young (3 months) and elderly (20–24 months) AE17 mesothelioma-bearing female C57BL/6J mice during tumor growth. Mesothelioma tumors grew faster in elderly compared with young mice, and this corresponded with an increase in tumor-associated macrophages. During healthy aging, macrophages increase in bone marrow and spleens suggesting that these sites have an increased potential to supply cancer-promoting macrophages. Interestingly, in tumor-bearing mice, bone marrow macrophages increased proliferation whilst splenic macrophages had reduced proliferation in elderly compared with young mice, and macrophage depletion using the F4/80 antibody slowed tumor growth in young and elderly mice. We also examined responses to treatment with intra-tumoral IL-2/anti-CD40 antibody immunotherapy and found it was less effective in elderly (38% tumor regression) compared to young mice (90% regression). Tumor-bearing elderly mice decreased in vivo anti-tumor cytotoxic T cell activity in tumor draining lymph nodes and spleens. Depletion of macrophages using F4/80 antibody in elderly, but not young mice, improved IL-2/anti-CD40 immunotherapy up to 78% tumor regression. Macrophage depletion also increased in vivo anti-tumor T cell activity in elderly, but not young mice. All the tumor-bearing elderly (but not young) mice had decreased body weight (i.e., exhibited cachexia), which was greatly exacerbated by immunotherapy; whereas macrophage depletion prevented this immunotherapy-induced cachexia. These studies strongly indicate that age-related changes in macrophages play a key role in driving cancer cachexia in the elderly, particularly during immunotherapy, and sabotage elderly anti-tumor immune responses.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 81%

Section: Introductionmentioning

confidence: 99%

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Macrophage Depletion in Elderly Mice Improves Response to Tumor Immunotherapy, Increases Anti-tumor T Cell Activity and Reduces Treatment-Induced Cachexia

et al. 2018

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“…26,27 CFSElabeled splenocytes were incubated for 2-4 h (37x C, 5% CO 2 ) to remove adherent macrophages and DCs and collect nonadherent cells (consisting of 40% T cells). Splenocytes were labeled with carboxyfluorescein diacetate succinimidyl ester (CFSE; Invitrogen) a fluorescent dye that binds permanently to cell membranes.…”

Section: Allogeneic Mixed Lymphocyte Reaction (Mlr)mentioning

confidence: 99%

“…3 Systemic injection of IL-2/CD40 was unacceptably toxic, even in young adult mice, and significantly less effective than intra-tumoral administration. 26,27 Others have shown that targeting and depleting tumor-associated macrophages inhibits mesothelioma tumor development. 3 The role of macrophages was not examined in those studies.…”

Section: Introductionmentioning

confidence: 99%

Murine mesothelioma induces locally-proliferating IL-10⁺TNF-α⁺CD206⁻CX3CR1⁺M3 macrophages that can be selectively depleted by chemotherapy or immunotherapy

et al. 2016

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We used a murine model to monitor changes to myeloid cell subsets, i.e., myeloid-derived suppressor cells (MDSCs), M1 macrophages that secrete pro-inflammatory cytokines and express CD40 and CD80 and suppressive M2 macrophages that secrete anti-inflammatory cytokines and express CD206 and CX3CR1, during mesothelioma progression and during chemotherapy or immunotherapy-induced tumor regression. In vitro studies showed that mesothelioma-conditioned media generated CD206(-)CX3CR1(+)MCP-1(+)TGF-β(+) macrophages that induced T cell proliferation but prevented T cell IFNγ production. In vivo studies showed that co-inoculation of macrophages with mesothelioma cells led to faster tumor growth, and depleting macrophages using anti-F4/80 antibody induced tumor regression. Flow cytometry revealed increasing levels of different suppressive myeloid cells in lymphoid organs: MDSCs dominated bone marrow (BM) and spleens, M2 macrophages dominated tumor-draining lymph nodes (DLN) and a mixed IL-10(+)TNF-α(+)CD206(-)CX3CR1(+) M1/M2 (M3) macrophage subset dominated the mesothelioma microenvironment. Ki67 staining and cell cycle analysis showed that tumor-associated M1 and M3, but not M2, macrophages were proliferating in situ, with M1 cells arrested in the G1 phase while M3 cells progressed to mitosis. Immunohistochemistry showed that M1 and M3 cells were co-located supporting the hypothesis that M1 cells transition to M3 cells during proliferation. Gemcitabine reduced tumor-associated M3 and MDSCs, but not M2 macrophages, the latter likely contributing to the tumor outgrowth seen following treatment cessation. In contrast, IL-2/agonist anti-CD40 antibody therapy reduced M3 cells and polarized macrophages into M1 cells coinciding with tumor regression. These data show that myeloid cells, particularly M3 cells, represent a therapeutic target for the generation of antitumor immunity.

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Aging and immunotherapies: New horizons for the golden ages

Hamilton

Henry

2020

Aging and Cancer

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The life expectancy of the world's elderly population (65 and older) continues to reach new milestones with older individuals currently comprising greater than 8.5% (617 million) of the world's population. This percentage is predicted to approach 20% of the world's population by 2050 (representing 1.6 billion people). Despite this amazing feat, many healthcare systems are not equipped to handle the multitude of diseases that commonly manifest with age, including most types of cancers. As the world's aging population grows, cancer treatments continue to evolve. Immunotherapies are a new drug class that has revolutionized our ability to treat previously intractable cancers; however, their efficacy in patients with compromised immune systems remains unclear. In this review, we will discuss how aging-associated losses in immune homeostasis impact the efficacy and safety of immunotherapy treatment in preclinical models of aging. We will also discuss how these findings translate to elderly patients receiving immunotherapy treatment for refractory and relapsed cancers, as well as, strategies that could be explored to improve the efficacy of immunotherapies in aged patients.

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IL-2/CD40-activated macrophages rescue age and tumor-induced T cell dysfunction in elderly mice

Cited by 24 publications

References 46 publications

Macrophage Depletion in Elderly Mice Improves Response to Tumor Immunotherapy, Increases Anti-tumor T Cell Activity and Reduces Treatment-Induced Cachexia

Macrophage Depletion in Elderly Mice Improves Response to Tumor Immunotherapy, Increases Anti-tumor T Cell Activity and Reduces Treatment-Induced Cachexia

Murine mesothelioma induces locally-proliferating IL-10⁺TNF-α⁺CD206⁻CX3CR1⁺M3 macrophages that can be selectively depleted by chemotherapy or immunotherapy

Aging and immunotherapies: New horizons for the golden ages

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IL-2/CD40-activated macrophages rescue age and tumor-induced T cell dysfunction in elderly mice

Cited by 24 publications

References 46 publications

Macrophage Depletion in Elderly Mice Improves Response to Tumor Immunotherapy, Increases Anti-tumor T Cell Activity and Reduces Treatment-Induced Cachexia

Macrophage Depletion in Elderly Mice Improves Response to Tumor Immunotherapy, Increases Anti-tumor T Cell Activity and Reduces Treatment-Induced Cachexia

Murine mesothelioma induces locally-proliferating IL-10+TNF-α+CD206−CX3CR1+M3 macrophages that can be selectively depleted by chemotherapy or immunotherapy

Aging and immunotherapies: New horizons for the golden ages

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Murine mesothelioma induces locally-proliferating IL-10⁺TNF-α⁺CD206⁻CX3CR1⁺M3 macrophages that can be selectively depleted by chemotherapy or immunotherapy