Rapid activation of tumor-associated macrophages boosts preexisting tumor immunity

Hoves, Sabine; Ooi, Chia Huey; Wolter, Carsten; Sade, Hadassah; Bissinger, Stefan; Schmittnaegel, Martina; Ast, Oliver; Giusti, Anna Maria; Wartha, Katharina; Runza, Valeria; Xu, Wei; Kienast, Yvonne; Cannarile, Michael A.; Levitsky, Hyam I.; Romagnoli, Solange; Palma, Michele De; Rüttinger, Dominik; Ries, Carola H.

doi:10.1084/jem.20171440

Cited by 159 publications

(143 citation statements)

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“…Other very recent studies have demonstrated interesting strategies for the in vivo modulation of TAMs. In a murine colon adenocarcinoma model, treatment with two mAbs to concomitantly block CSF‐1R and stimulate CD40 resulted in the reprogramming of TAMs by increasing pro‐inflammatory signals such as IL‐12B, IL‐27, IL‐1β and CCL5 . In addition, in a melanoma tumor model, the depletion of CD163 + TAMs, using an anti‐CD163 antibody conjugated to a doxorubicin charged liposome, led to a monocyte influx, the up‐regulation of IFN‐related cytokines and an anti‐tumor T‐cell response …”

Section: Discussionmentioning

confidence: 99%

“…In a murine colon adenocarcinoma model, treatment with two mAbs to concomitantly block CSF-1R and stimulate CD40 resulted in the reprogramming of TAMs by increasing pro-inflammatory signals such as IL-12B, IL-27, IL-1b and CCL5. 44 In addition, in a melanoma tumor model, the depletion of CD163 + TAMs, using an anti-CD163 antibody conjugated to a doxorubicin charged liposome, led to a monocyte influx, the up-regulation of IFN-related cytokines and an anti-tumor T-cell response. 45 Importantly, we described for the first time that conditioned-media supernatants of dilacerated primary human breast tumors promote either highly suppressive CD163 high IL-10 high CD86 low MΦ, resembling suppressive TAMs, [46][47][48] or CD163 low IL-10 low CD86 low MΦ, displaying moderate suppressive functions.…”

Section: Discussionmentioning

confidence: 99%

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CD163⁺ tumor‐associated macrophage accumulation in breast cancer patients reflects both local differentiation signals and systemic skewing of monocytes

et al. 2020

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Objectives The accumulation of tumor‐associated macrophages (TAMs) is correlated with poor clinical outcome, but the mechanisms governing their differentiation from circulating monocytes remain unclear in humans. Methods Using multicolor flow cytometry, we evaluated TAMs phenotype in 93 breast cancer (BC) patients. Furthermore, monocytes from healthy donors were cultured in the presence of supernatants from dilacerated primary tumors to investigate their differentiation into macrophages (MΦ) in vitro. Additionally, we used transcriptomic analysis to evaluate BC patients’ blood monocytes profiles. Results We observed that high intra‐tumor CD163‐expressing TAM density is predictive of reduced survival in BC patients. In vitro, M‐CSF, TGF‐β and VEGF from primary tumor supernatants skewed the differentiation of healthy donor blood monocytes towards CD163highCD86lowIL‐10high M2‐like MΦ that strongly suppressed CD4+ T‐cell expansion via PD‐L1 and IL‐10. In addition, blood monocytes from about 40% of BC patients displayed an altered response to in vitro stimulation, being refractory to type‐1 MΦ (M1‐MΦ) differentiation and secreting higher amounts of immunosuppressive, metastatic‐related and angiogenic cytokines. Aside from showing that monocyte transcriptome is significantly altered by the presence of BC, we also demonstrated an overall metabolic de‐activation in refractory monocytes of BC patients. In contrast, monocytes from sensitive BC patients undergoing normal M1‐MΦ differentiation showed up‐regulation of IFN‐response genes and had no signs of metabolic alteration. Conclusion Altogether, our results suggest that systemic factors skew BC patient blood monocytes towards a pro‐metastatic profile, resulting in the accumulation of further polarised CD163high TAMs resembling type‐2 MΦ (M2‐MΦ) in the local BC microenvironment. These data indicate that monitoring circulating monocytes in BC patients may provide an indication of early systemic alterations induced by cancer and, thus, be instrumental in the development of improved personalised immunotherapeutic interventions.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

CD163⁺ tumor‐associated macrophage accumulation in breast cancer patients reflects both local differentiation signals and systemic skewing of monocytes

et al. 2020

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“…Repolarized TAMs could therefore become efficient antigen-presenting cells activating CD8 and CD4 T cells in situ (21). TAM repolarization strategies include agonistic anti-CD40 (aCD40), blockade of CSF1 signaling, selective inhibition of PI3Kg, deletion of Dicer, as well as targeting surface markers expressed by suppressive macrophages (2,8,16,(21)(22)(23)(24)(25)(26)(27)(28). Repolarization and depletion have recently been combined to achieve an optimal stimulatory phenotype on macrophages; however, its implication on tumor sensitization to checkpoint inhibitors remains unclear (27).…”

Section: Introductionmentioning

confidence: 99%

Anti–PD-L1 Treatment Results in Functional Remodeling of the Macrophage Compartment

Xiong¹,

Mittman²,

Rodriguez³

et al. 2019

Cancer Research

136

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© 2019 American Association for Cancer Research T cells T cells aPDL1 MHCI and MHCII ARGI iNOS CD40 CD86 proinflammatory cytokines Phagocytosis pathways Proinflammatory Suppressive MacrophageWithout treatment, tumor macrophages maintain a suppressive phenotype.Following anti-PD-L1 treatment, increased IFN signaling remodels the macrophage compartment towards a more proinflammatory phenotype, which can enhance T-cell responses.Remodeling of the macrophage compartment is driven by IFN following anti-PD-L1 treatment. Macrophage Cancer cells ARGI IFNγIFNγ Checkpoint inhibitors like anti-PD1/PD-L1 have demonstrated significant therapeutic efficacy in a subset of patients partly through reinvigoration of CD8 T cells. However, their impact on myeloid cells remains largely unknown. Here, we report that anti-PD-L1 treatment favorably impacts the phenotype and function of tumor macrophages by polarizing the macrophage compartment toward a more proinflammatory phenotype. This phenotype was characterized by a decrease in Arginase-I (ARG1) expression and an increase in iNOS, MHCII, and CD40 expression. Whole-transcriptome profiling further confirmed extensive polarization of both tumor monocytes and macrophages from a suppressive to a proinflammatory, immunostimulatory phenotype. This polarization was driven mainly through IFNg and was associated with enhanced T-cell activity. Transfer of monocytes into anti-PD-L1treated tumor-bearing mice led to macrophage differentiation into a more proinflammatory phenotype, with an increase in CD8 T cells expressing granzyme-B and an increase in the CD8/Treg ratio compared with control-treated mice. Although in responsive tumor models, anti-PD-L1 treatment remodeled the macrophage compartment with beneficial effects on T cells, both macrophage reprogramming and depletion were needed to maximize anti-PD-L1 responses in a tumor immune contexture with high macrophage burden. Our results demonstrate that anti-PD-L1 treatment can favorably remodel the macrophage compartment in responsive tumor models toward a more proinflammatory phenotype, mainly through increased IFNg levels. They also suggest that directly targeting these cells with reprogramming and depleting agents may further augment the breadth and depth of response to anti-PD-L1 treatment in less responsive or more macrophage-dense tumor microenvironments.

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“…We assessed the ability of JHU083 to inhibit growth of EO771, which is similar to 4T1 triple negative breast cancer. The EO771 tumor model is moderately sensitive to immunotherapy in the form of anti-PD1 monotherapy or anti-CSF1R + anti-CD40 combination immunotherapy (Hoves et al, 2018). We observed significant inhibition of tumor growth and enhanced survival with JHU083 treatment alone (Supplementary figure 6A and B).…”

Section: The Glutamine Antagonist Jhu083 Enhances the Efficacy Of Chementioning

confidence: 71%

“…Recently, multiple studies have demonstrated that pro-inflammatory TAMs inhibit tumor growth (Hoves et al, 2018;Perry et al, 2018). Our RNA sequencing data of TAMs from JHU083 treated mice demonstrated an increase in the pro-inflammatory cytokine, Tnf.…”

Section: Targeting Glutamine Metabolism Promotes the Reprogramming Ofmentioning

confidence: 72%

Targeting glutamine metabolism enhances tumor specific immunity by inhibiting the generation of MDSCs and reprogramming tumor associated macrophages

Sun

Zhao

et al. 2019

Preprint

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Rapid activation of tumor-associated macrophages boosts preexisting tumor immunity

Cited by 159 publications

References 71 publications

CD163⁺ tumor‐associated macrophage accumulation in breast cancer patients reflects both local differentiation signals and systemic skewing of monocytes

CD163⁺ tumor‐associated macrophage accumulation in breast cancer patients reflects both local differentiation signals and systemic skewing of monocytes

Anti–PD-L1 Treatment Results in Functional Remodeling of the Macrophage Compartment

Targeting glutamine metabolism enhances tumor specific immunity by inhibiting the generation of MDSCs and reprogramming tumor associated macrophages

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Rapid activation of tumor-associated macrophages boosts preexisting tumor immunity

Cited by 159 publications

References 71 publications

CD163+ tumor‐associated macrophage accumulation in breast cancer patients reflects both local differentiation signals and systemic skewing of monocytes

CD163+ tumor‐associated macrophage accumulation in breast cancer patients reflects both local differentiation signals and systemic skewing of monocytes

Anti–PD-L1 Treatment Results in Functional Remodeling of the Macrophage Compartment

Targeting glutamine metabolism enhances tumor specific immunity by inhibiting the generation of MDSCs and reprogramming tumor associated macrophages

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CD163⁺ tumor‐associated macrophage accumulation in breast cancer patients reflects both local differentiation signals and systemic skewing of monocytes

CD163⁺ tumor‐associated macrophage accumulation in breast cancer patients reflects both local differentiation signals and systemic skewing of monocytes