MITF and c-Jun antagonism interconnects melanoma dedifferentiation with pro-inflammatory cytokine responsiveness and myeloid cell recruitment

Riesenberg, Stefanie; Groetchen, Angela; Siddaway, Robert; Bald, Tobias; Reinhardt, Julia; Smorra, Denise; Kohlmeyer, Judith; Renn, Marcel; Phung, Bengt; Aymans, Pia; Schmidt, Tobias; Hornung, Veit; Davidson, Irwin; Goding, Colin R.; Jönsson, Göran; Landsberg, Jennifer; Tüting, Thomas; Hölzel, Michael

doi:10.1038/ncomms9755

Cited by 178 publications

(203 citation statements)

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“…Smith et al (2014) reported that TNFα promotes melanoma growth and therapeutic resistance by up-regulating MITF, which should promote differentiation. In contrast, other studies report that TNFα down-regulates MITF (Landsberg et al 2012;Konieczkowski et al 2014;Riesenberg et al 2015), decreases differentiation, and promotes a slow-cycling phenotype (Ostyn et al 2014), a characteristic of MITF-low cells (Cheli et al 2011b). Significantly, a recently described melanoma TNFα response gene set (Riesenberg et al 2015) positively correlated with the GSS score in the TCGA melanoma cohort as well as the single-cell RNA-seq patient-derived melanoma data from Tirosh et al (2016) (Fig.…”

Section: Inhibition Of Eif2b Drives Invasivenessmentioning

confidence: 88%

“…The moving average expression of individual genes of interest or averaged signatures were calculated using a sample window size of n = 20, and trend lines were added to the bar plots. An R-skript for calculating and generating moving average plots of TCGA cancer cohorts implementing TCGA access via cBioportal was provided in our previous study (Riesenberg et al 2015). Significance of the Spearman rank correlation was determined by an asymptotic Spearman correlation test using the original log 2 expression values and not the moving average values.…”

Section: Tcga Transcriptomic Analysismentioning

confidence: 99%

“…However, while short-term depletion of MITF leads to invasiveness and adoption of a tumor-initiating phenotype (Cheli et al 2011b), longer-term MITF depletion leads to senescence (Giuliano et al 2010). However, in vivo senescence is largely restricted to nevi (Michaloglou et al 2005;Gray-Schopfer et al 2006), although melanomas can contain many MITF-negative cells (Goodall et al 2008;Riesenberg et al 2015). How MITF is downregulated in vivo without provoking senescence is unknown, but low MITF is correlated with resistance to MEK and BRAF inhibitors (Konieczkowski et al 2014;Muller et al 2014;Dugo et al 2015).…”

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confidence: 99%

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Translation reprogramming is an evolutionarily conserved driver of phenotypic plasticity and therapeutic resistance in melanoma

et al. 2017

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The intratumor microenvironment generates phenotypically distinct but interconvertible malignant cell subpopulations that fuel metastatic spread and therapeutic resistance. Whether different microenvironmental cues impose invasive or therapy-resistant phenotypes via a common mechanism is unknown. In melanoma, low expression of the lineage survival oncogene microphthalmia-associated transcription factor (MITF) correlates with invasion, senescence, and drug resistance. However, how MITF is suppressed in vivo and how MITF-low cells in tumors escape senescence are poorly understood. Here we show that microenvironmental cues, including inflammationmediated resistance to adoptive T-cell immunotherapy, transcriptionally repress MITF via ATF4 in response to inhibition of translation initiation factor eIF2B. ATF4, a key transcription mediator of the integrated stress response, also activates AXL and suppresses senescence to impose the MITF-low/AXL-high drug-resistant phenotype observed in human tumors. However, unexpectedly, without translation reprogramming an ATF4-high/MITF-low state is insufficient to drive invasion. Importantly, translation reprogramming dramatically enhances tumorigenesis and is linked to a previously unexplained gene expression program associated with anti-PD-1 immunotherapy resistance. Since we show that inhibition of eIF2B also drives neural crest migration and yeast invasiveness, our results suggest that translation reprogramming, an evolutionarily conserved starvation response, has been hijacked by microenvironmental stress signals in melanoma to drive phenotypic plasticity and invasion and determine therapeutic outcome.

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Section: Inhibition Of Eif2b Drives Invasivenessmentioning

confidence: 88%

Section: Tcga Transcriptomic Analysismentioning

confidence: 99%

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confidence: 99%

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Translation reprogramming is an evolutionarily conserved driver of phenotypic plasticity and therapeutic resistance in melanoma

et al. 2017

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“…49 MITF also repressed ZEB1 transcription in the 501mel human melanoma cell line, 50 as well as inflammation genes through repressing c-Jun expression in mouse and human melanoma cell lines. 51 MITF recruits RBPJK as a cofactor in repressing transcription of microRNAs miR-221 and miR-222 in human melanoma cell lines. 52 It remains mechanistically unclear how MITF represses target genes and what functional roles MITF has through repressing gene expression.…”

Section: Mitf Target Genesmentioning

confidence: 99%

The master role of microphthalmia-associated transcription factor in melanocyte and melanoma biology

Kawakami

Fisher

2017

Laboratory Investigation

205

162

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Certain transcription factors have vital roles in lineage development, including specification of cell types and control of differentiation. Microphthalmia-associated transcription factor (MITF) is a key transcription factor for melanocyte development and differentiation. MITF regulates expression of numerous pigmentation genes to promote melanocyte differentiation, as well as fundamental genes for maintaining cell homeostasis, including genes encoding proteins involved in apoptosis (eg, BCL2) and the cell cycle (eg, CDK2). Loss-of-function mutations of MITF cause Waardenburg syndrome type IIA, whose phenotypes include depigmentation due to melanocyte loss, whereas amplification or specific mutation of MITF can be an oncogenic event that is seen in a subset of familial or sporadic melanomas. In this article, we review basic features of MITF biological function and highlight key unresolved questions regarding this remarkable transcription factor.

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“…46,47 Furthermore, repression of MITF expression could make melanoma to recruit myeloid immune cells into the tumor microenvironment which could counteract tumor growth promoting and immunosuppressive functions. 48 Besides, MITF was related to intrinsic drug resistance and the drug resistance to BRAF inhibitors in melanoma cells, which could further promote cell survival and proliferation. 49,50 Melanoma cells expressing MITF highly displayed significant drug resistance in BRAF-i and MEK-i treatment.…”

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confidence: 99%

Cuprous oxide nanoparticle-inhibited melanoma progress by targeting melanoma stem cells

Wang²,

et al. 2017

IJN

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Recent studies have shown that metal and metal oxide have a potential function in antitumor therapy. Our previous studies demonstrated that cuprous oxide nanoparticles (CONPs) not only selectively induce apoptosis of tumor cells in vitro but also inhibit the growth and metastasis of melanoma by targeting mitochondria with little hepatic and renal toxicities in mice. As a further study, our current research revealed that CONPs induced apoptosis of human melanoma stem cells (CD271 +/high cells) in A375 and WM266-4 melanoma cell lines and could significantly suppress the expression of MITF, SOX10 and CD271 involved in the stemness maintenance and tumorigenesis of melanoma stem cells. CD271 +/high cells could accumulate more CONPs than CD271 −/low through clathrin-mediated endocytosis. In addition, lower dosage of CONPs exhibited good anti-melanoma effect by decreasing the cell viability, stemness and tumorigenesis of A375 and WM266-4 cells through reducing the expression of SOX10, MITF, CD271 and genes in MAPK pathway involved in tumor progression. Finally, CONPs obviously suppressed the growth of human melanoma in tumor-bearing nonobese diabetic-severe combined immunodeficiency (NOD-SCID) mice, accompanied with tumors structural necrosis and fibrosis remarkably and decreased expression of CD271, SOX10 and MITF. These results above proved the effectiveness of CONPs in inhibiting melanoma progress through multiple pathways, especially through targeting melanoma stem cells.

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MITF and c-Jun antagonism interconnects melanoma dedifferentiation with pro-inflammatory cytokine responsiveness and myeloid cell recruitment

Cited by 178 publications

References 70 publications

Translation reprogramming is an evolutionarily conserved driver of phenotypic plasticity and therapeutic resistance in melanoma

Translation reprogramming is an evolutionarily conserved driver of phenotypic plasticity and therapeutic resistance in melanoma

The master role of microphthalmia-associated transcription factor in melanocyte and melanoma biology

Cuprous oxide nanoparticle-inhibited melanoma progress by targeting melanoma stem cells

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