Tumor-Induced Tolerance and Immune Suppression Depend on the C/EBPβ Transcription Factor

Marigo, Ilaria; Bosio, Erika; Solito, Samantha; Mesa, Circe; Fernández, Audry; Dolcetti, Luigi; Ugel, Stefano; Sonda, Nada; Bicciato, Silvio; Falisi, Erika; Calabrese, Fiorella; Basso, Giuseppe; Zanovello, Paola; Cozzi, Emanuele; Mandruzzato, Susanna; Bronte, Vincenzo

doi:10.1016/j.immuni.2010.05.010

Cited by 768 publications

(846 citation statements)

References 35 publications

(52 reference statements)

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“…Bone marrow cells were cultured in the presence of GM-CSF and IL-6 as previously described. 15 After 4 d, most cells showed double expression of Gr1 and CD11b and strongly suppressed T-cell proliferation. These bone marrow-derived MDSC (BM-MDSC) were stimulated in culture with R848 for 48 h. As seen previously with MDSC following TLR7 treatment in vivo, we observed an increase in differentiation markers (F4/80 and CD11c) and maturation markers (MHC-I and MHC-II) on BM-MDSC upon in vitro R848 stimulation (Fig.…”

Section: Direct Tlr7 Stimulation Of Mdsc Induces Their Maturation Andmentioning

confidence: 96%

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TLR7-based cancer immunotherapy decreases intratumoral myeloid-derived suppressor cells and blocks their immunosuppressive function

et al. 2016

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Myeloid-derived suppressor cells (MDSC) are a heterogeneous population of immature myeloid cells with the capacity to inhibit immunological responses. During cancer progression, MDSC are recruited to the tumor sites and secondary lymphoid organs, leading to the suppression of the antitumor function of NK and T cells. Here, we show that the TLR7/8 agonist resiquimod (R848) has a direct effect on MDSC populations in tumor-bearing mice. Systemic application of R848 led to a rapid reduction in both intratumoral and circulating MDSC. The subpopulation of monocytic MDSC (m-MDSC) was the most affected by R848 treatment with an up to 5-fold decrease in the tumor. We found that TLR7 stimulation in tumor-bearing mice led to a maturation and differentiation of MDSC with upregulation of the surface molecules CD11c, F4/80, MHC-I, and MHC-II. MDSC treated with R848 lost their immunosuppressive function and acquired instead an antigen-presenting phenotype with the capability to induce specific Tcell proliferation. Importantly, we found that MDSC co-injected s.c. with CT26 tumor cells lost their ability to support tumor growth after pretreatment with R848. Our results demonstrate that treatment of tumorbearing mice with a TLR7/8 agonist acts directly on MDSC to induce their maturation and leads them to acquire a non-suppressive status. Considering the obstacles posed by MDSC for cancer immunotherapy, targeting these cells by a TLR7/8 agonist may improve immune responses against cancer.

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Section: Direct Tlr7 Stimulation Of Mdsc Induces Their Maturation Andmentioning

confidence: 96%

“…15 After red blood cell lysis (BD Pharm Lyse, BD Biosciences), cells were cultured in complete medium supplemented with 40 ng/mL GM-CSF and 40 ng/mL IL-6 (both from PeproTech, Rocky Hill, NJ) and harvested at day 4. The percentage of Gr1 C CD11b C cells was over 90%.…”

Section: Preparation Of Bone Marrow-derived Mdsc (Bm-mdsc)mentioning

confidence: 99%

TLR7-based cancer immunotherapy decreases intratumoral myeloid-derived suppressor cells and blocks their immunosuppressive function

et al. 2016

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“…More recently, C/EBPb was proposed as another transcription factor for the activation and functional suppression of MDSCs. 23 Although the role of STAT3 in C/ EBPb expression is not known, the requirement of IL-6 for the in vitro generation of immunosuppressive MDSCs suggests that STAT3 activation might be required for C/EBPb-dependent immunosuppression by MDSCs.…”

Section: Discussionmentioning

confidence: 99%

“…22 Additionally, C/EBPb has been suggested to be a master regulator for the immunosuppressive function of MDSCs. 23 We hypothesized that while TLR ligation on effector cells is indispensible for the successful eradication of the tumor, Myd88 signaling in MDSCs might mediate suppressive function. In this study, we investigated the role of Myd88 in the immunosuppressive function of MDSCs against CD4 þ and CD8 þ T cells and assessed methods to block the Myd88-mediated suppressive function of MDSCs without inhibiting effector cells.…”

mentioning

confidence: 99%

Blockade of Myd88 signaling induces antitumor effects by skewing the immunosuppressive function of myeloid‐derived suppressor cells

Hong

Chang

Lee

et al. 2012

Intl Journal of Cancer

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Myd88 is an important adaptor molecule for the activation of NADPH oxidase and arginase-1, which are responsible for the suppressive function of myeloid-derived suppressor cells (MDSCs). When wild-type and Myd88 2/2 mice were subcutaneously injected with CT26 colon cancer cells expressing human Her-2/neu, tumor growth was retarded in Myd88 2/2 mice than in wild-type mice. Although the generation of CD11b 1 Gr-1 1 MDSCs was less in Myd88 2/2 mice than in wild-type mice, Myd88 2/2 mice having tumor masses still had significant quantities of MDSCs, suggesting that MDSC generation might be independent of Myd88 signaling. However, MDSCs obtained from tumor-bearing Myd88 2/2 mice failed to suppress antigenspecific proliferation of CD8 1 T cells and CD4 1 T cells, whereas MDSCs from wild-type mice significantly suppressed both types of T cells. Consistent with this, we found that the levels of costimulatory molecules and MHC class II were significantly increased in MDSCs obtained from Myd88 2/2 mice compared with wild-type mice after tumor challenge. Furthermore, CD4 1 T cells residing in tumor-draining lymph nodes of Myd88 2/2 mice secreted more TNF-a than those of wild-type mice. Finally, the blockade of Myd88 signaling by treatment with Myd88 inhibitory peptide, during later tumor stages, significantly inhibited the growth of immunogenic tumors. Overall, these data suggest that signaling through the Myd88 adaptor molecule is critical for the direct suppressive function of MDSCs and approaches to block Myd88-mediated signaling in MDSCs might be effective to inhibit the immunosuppressive function of MDSCs.

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“…In turn, the increase in S100A8 and S100A9 inhibits dendritic cell differentiation and promotes the MDSC expansion, accumulation, and the recruitment the MDSCs to the tumor site (Cheng et al 2008). CCAATenhancer-binding protein b which is reported as a crucial factor for the MDSC expansion is also upregulated by STAT3 (Marigo et al 2010). In addition, STAT3 increases the transcription of p47 phox which is a component of nicotinamide adenine dinucleotide phosphate oxidase (NOX2).…”

Section: Expansion and Activation Of Mdscsmentioning

confidence: 99%

Phenotypic and functional dissection of myeloid-derived suppressor cells

Han

Yang

2016

Appl Biol Chem

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Myeloid-derived suppressor cells (MDSCs) are originated and differentiated population from common hematopoietic progenitor cells. Generally, in the late stage of inflammation, MDSCs differentiation and expansion are promoted to suppress the over-activated immune system so that the immune system can maintain the homeostasis. Recently, it has been revealed that MDSCs accumulate in cancer patients and tumor-bearing experimental animals, and these tumor-derived MDSCs suppress anti-tumor immunity by secreting immunosuppressive cytokines including reactive oxygen species and inducible nitric oxide synthase. This fact prompts scientists to shed light on MDSCs as significant targets for anti-cancer immunotherapy. However, due to morphological, phenotypic, and functional heterogeneities of MDSCs, it is not easy to develop therapeutic strategies targeting MDSCs. In this review, we will summarize recent progress on defined subsets of MDSCs and their strategies to suppress T cellmediated anti-tumor immunity.

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Tumor-Induced Tolerance and Immune Suppression Depend on the C/EBPβ Transcription Factor

Cited by 768 publications

References 35 publications

TLR7-based cancer immunotherapy decreases intratumoral myeloid-derived suppressor cells and blocks their immunosuppressive function

TLR7-based cancer immunotherapy decreases intratumoral myeloid-derived suppressor cells and blocks their immunosuppressive function

Blockade of Myd88 signaling induces antitumor effects by skewing the immunosuppressive function of myeloid‐derived suppressor cells

Phenotypic and functional dissection of myeloid-derived suppressor cells

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