MYC inhibition reprograms tumor immune microenvironment by recruiting T lymphocytes and activating the CD40/CD40L system in osteosarcoma

Jiang, Kuo; Zhang, Qian‐Feng; Fan, Yingli; Li, Jia; Zhang, Jitao; Wang, Wentao; Fan, Jinzhu; Guo, Yunshan; Liu, Shichang; Hao, Ding-Jun; Wang, Yongxiang; Wang, Lei; Shan, Lequn

doi:10.1038/s41420-022-00923-8

Cited by 16 publications

(16 citation statements)

References 40 publications

(47 reference statements)

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“…Myc expression in TAMs has been shown to regulate tumor growth by reinforcing an immunosuppressive microenvironment [ 13 , 14 , 30 ], while the inhibition of Myc enables T-cell-mediated immune surveillance [ 31 , 32 ]. We therefore profiled tumors from Gp130 F/F , KPT, B16F10, or MC38 models that arose in either LysM +/+ ; Myc fl/fl or LysM Cre/+ ; Myc fl/fl hosts for markers associated with immune suppression (i.e., Il4 , Il10 , Il13 , Arg1 , Ym1 , Mrc1 , Tgfβ ) and immune activation (i.e., Il1β , Il12 , Tnfα , Nos2 , Ifnγ , GzmB and Prf1 ).…”

Section: Resultsmentioning

confidence: 99%

Tumor Growth Remains Refractory to Myc Ablation in Host Macrophages

Morrow

Allam

Konecnik

et al. 2022

Cells

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Aberrant expression of the oncoprotein c-Myc (Myc) is frequently observed in solid tumors and is associated with reduced overall survival. In addition to well-recognized cancer cell-intrinsic roles of Myc, studies have also suggested tumor-promoting roles for Myc in cells of the tumor microenvironment, including macrophages and other myeloid cells. Here, we benchmark Myc inactivation in tumor cells against the contribution of its expression in myeloid cells of murine hosts that harbor endogenous or allograft tumors. Surprisingly, we observe that LysMCre-mediated Myc ablation in host macrophages does not attenuate tumor growth regardless of immunogenicity, the cellular origin of the tumor, the site it develops, or the stage along the tumor progression cascade. Likewise, we find no evidence for Myc ablation to revert or antagonize the polarization of alternatively activated immunosuppressive macrophages. Thus, we surmise that systemic targeting of Myc activity may confer therapeutic benefits primarily through limiting Myc activity in tumor cells rather than reinvigorating the anti-tumor activity of macrophages.

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Section: Resultsmentioning

confidence: 99%

Tumor Growth Remains Refractory to Myc Ablation in Host Macrophages

Morrow

Allam

Konecnik

et al. 2022

Cells

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“…MYC activation induces the expression of p16 (INK4a) and p21 (Cip1) and resulted in Cdk2-deficient CS [ 31 ]. Inhibition of MYC reprograms TME by recruiting T lymphocytes and activating the CD40/CD40L system in osteosarcoma [ 32 ]. Overexpressed distal-less homeobox 2 (DLX2) is associated with adverse clinical outcomes in hepatocellular carcinoma [ 33 ] and gastric adenocarcinoma [ 34 ].…”

Section: Discussionmentioning

confidence: 99%

Subtype Classification and Prognosis Signature Construction of Osteosarcoma Based on Cellular Senescence-Related Genes

Wang

Liu

Wang

et al. 2022

Journal of Oncology

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Background. Cellular senescence (CS) is an alternative procedure that replaces or reinforces inadequate apoptotic responses and is used as an influencing factor for a variety of cancers. The value of CS gene in evaluating the immunotherapy response and clinical outcome of osteosarcoma (OS) has not been reported, and an accurate risk model based on CS gene has not been developed for OS patients. Methods. 279 CS genes were obtained from CellAge. Univariate Cox regression analysis was used to screen the CS gene which was significantly related to the prognosis of OS samples in TARGET data set. The prognosis, clinicopathological features, immune infiltration, gene expression at immune checkpoints, tumor immune dysfunction and exclusion (TIDE) score, and chemotherapy resistance of OS were analyzed among clusters. Least absolute shrinkage and selection operator (Lasso) Cox regression analysis to build cellular senescence-related gene signature (CSRS). Univariate and multivariate Cox regression analysis of CSRS and clinical parameters were carried out, and the parameters with independent prognostic value were used to construct nomogram. Results. Based on 30 CS genes related to OS prognosis, OS samples were divided into three clusters: C1, C2, and C3. C3 showed the lowest survival rate and metastasis rate and the highest immune score and stromal score and was more likely to respond to immune checkpoint blockade (ICB) treatment. A CSRS scoring system including four CS genes (MYC, DLX2, EPHA3, and LIMK1) was constructed, which could distinguish the survival outcome, tumor microenvironment (TME) status, and ICB treatment response of patients with different CSRS score. Nomogram constructed by CSRS score and metastatic has a high prognostic value for OS. Conclusions. Our study identified a molecular classification determined by CS-related genes and developed a new CSRS that has potential value in OS immunotherapy response and clinical outcome prediction.

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“…In addition, the CD40/CD40L immune checkpoint pathway, which rescues tumour cells from apoptosis, prolongs survival and enhances the proliferation, activation, or maturation of APCs, including primarily macrophages and DCs, to produce IL-12 or IL-18 to stimulate NK cells. These, in turn, produce IFN-γ and express co-stimulatory molecules, such as CD80/CD86, ICAM-1, and CD44, which are required for the non-energetic full activation of T cells following T cell receptor stimulation [ 281 , 282 ].…”

Section: Ev-based Vaccine Therapy For Cancermentioning

confidence: 99%

Regulation of Extracellular Vesicle-Mediated Immune Responses against Antigen-Specific Presentation

Matsuzaka

Yashiro

2022

Vaccines

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Extracellular vesicles (EVs) produced by various immune cells, including B and T cells, macrophages, dendritic cells (DCs), natural killer (NK) cells, and mast cells, mediate intercellular communication and have attracted much attention owing to the novel delivery system of molecules in vivo. DCs are among the most active exosome-secreting cells of the immune system. EVs produced by cancer cells contain cancer antigens; therefore, the development of vaccine therapy that does not require the identification of cancer antigens using cancer-cell-derived EVs may have significant clinical implications. In this review, we summarise the molecular mechanisms underlying EV-based immune responses and their therapeutic effects on tumour vaccination.

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MYC inhibition reprograms tumor immune microenvironment by recruiting T lymphocytes and activating the CD40/CD40L system in osteosarcoma

Cited by 16 publications

References 40 publications

Tumor Growth Remains Refractory to Myc Ablation in Host Macrophages

Tumor Growth Remains Refractory to Myc Ablation in Host Macrophages

Subtype Classification and Prognosis Signature Construction of Osteosarcoma Based on Cellular Senescence-Related Genes

Regulation of Extracellular Vesicle-Mediated Immune Responses against Antigen-Specific Presentation

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