Human melanocyte development and melanoma dedifferentiation at single-cell resolution

Belote, R.L.; Le, Daniel; Maynard, Ashley; Lang, Ursula E.; Sinclair, Adriane; Lohman, Brian K.; Planells-Palop, Vicente; Baskin, Laurence S.; Tward, Aaron D.; Darmanis, Spyros; Judson-Torres, Robert L.

doi:10.1038/s41556-021-00740-8

Cited by 63 publications

(74 citation statements)

References 86 publications

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“…Sequencing data represented in ( A–F ) are from n=3 per condition analyzed with DESeq2. ( F ) Gene set enrichment analysis (GSEA) comparing DE gene sets from ( D ) to Molecular Signature Database Hallmark gene sets, KEGG Pathway gene sets and published signatures of melanocyte signaling and differentiation from Belote et al, 2021 ; Tsoi et al, 2018 ; Tirosh et al, 2016 ; Ryu et al, 2011 ; Hoek and Goding, 2010 . All enrichments with adjusted p value<0.025 are depicted.…”

Section: Resultsmentioning

confidence: 99%

“…We next conducted gene set enrichment analyses (GSEA) comparing TPA-regulated genes and BRAF V600E - regulated genes to Molecular Signature Database Hallmark gene sets ( Liberzon et al, 2015 ), the KEGG PATHWAY database ( Kanehisa et al, 2016 ), and signatures important in BRAF V600E signaling ( Ryu et al, 2011 ), human melanocyte differentiation ( Belote et al, 2021 ), or melanoma cell state ( Hoek and Goding, 2010 ; Tirosh et al, 2016 ; Tsoi et al, 2018 ). Among the pathways uniquely enriched with BRAF V600E expression were the expected increases in signatures downstream of BRAF V600E , MAPK (KRAS) signaling, and glycolysis ( Haq et al, 2014 ; Figure 4F and Supplementary file 6 ).…”

Section: Resultsmentioning

confidence: 99%

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BRAFV600E induces reversible mitotic arrest in human melanocytes via microRNA-mediated suppression of AURKB

McNeal

Belote

Zeng

et al. 2021

eLife

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Benign melanocytic nevi frequently emerge when an acquired BRAFV600E mutation triggers unchecked proliferation and subsequent arrest in melanocytes. Recent observations have challenged the role of oncogene-induced senescence in melanocytic nevus formation, necessitating investigations into alternative mechanisms for the establishment and maintenance of proliferation arrest in nevi. We compared the transcriptomes of melanocytes from healthy human skin, nevi, and melanomas arising from nevi and identified a set of microRNAs as highly expressed nevus-enriched transcripts. Two of these microRNAs—MIR211-5p and MIR328-3p—induced mitotic failure, genome duplication, and proliferation arrest in human melanocytes through convergent targeting of AURKB. We demonstrate that BRAFV600E induces a similar proliferation arrest in primary human melanocytes that is both reversible and conditional. Specifically, BRAFV600E expression stimulates either arrest or proliferation depending on the differentiation state of the melanocyte. We report genome duplication in human melanocytic nevi, reciprocal expression of AURKB and microRNAs in nevi and melanomas, and rescue of arrested human nevus cells with AURKB expression. Taken together, our data describe an alternative molecular mechanism for melanocytic nevus formation that is congruent with both experimental and clinical observations.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

BRAFV600E induces reversible mitotic arrest in human melanocytes via microRNA-mediated suppression of AURKB

McNeal

Belote

Zeng

et al. 2021

eLife

Self Cite

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“…Prior studies comparing melanocytes and cutaneous melanoma cells have reported on coding mutations, gene expression changes only, or have used human or zebrafish cell lines rather than focusing on in vivo animal models ( Yen et al 2013 ; Haltaufderhyde and Oancea 2014 ; Kaufman et al 2016 ; Badal et al 2017 ; Kunz et al 2018 ; Venkatesan et al 2018 ; Marie et al 2020 ; Wouters et al 2020 ). Single-cell RNA-seq experiments so far generally focus on the heterogeneity within cell populations, rather than a comparison between melanocytes and melanoma cells, or they do not evaluate the epigenetic landscape ( Ennen et al 2015 ; Tirosh et al 2016 ; Gan et al 2018 ; Rambow et al 2018 ; Baron et al 2020 ; Li et al 2020 ; Belote et al 2021 ; Travnickova and Patton 2021 ). Thus, we sought to characterize the epigenetic and transcriptional differences between zebrafish nonmalignant, precancerous, and malignant melanocytes in a genetically defined melanoma context.…”

Section: Introductionmentioning

confidence: 99%

Transcriptional profile and chromatin accessibility in zebrafish melanocytes and melanoma tumors

Kramer

Godoy

Kaufman

2021

G3 Genes|Genomes|Genetics

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Transcriptional and epigenetic characterization of melanocytes and melanoma cells isolated from their in vivo context promises to unveil key differences between these developmentally related normal and cancer cell populations. We therefore engineered an enhanced Danio rerio (zebrafish) melanoma model with fluorescently labeled melanocytes to allow for isolation of normal (wild type) and premalignant (BRAFV600E-mutant) populations for comparison to fully transformed BRAFV600E-mutant, p53 loss-of-function melanoma cells. Using fluorescence activated cell sorting to isolate these populations, we performed high-quality RNA-seq and ATAC-seq on sorted zebrafish melanocytes vs. melanoma cells, which we provide as a resource here. Melanocytes had consistent transcriptional and accessibility profiles, as did melanoma cells. Comparing melanocytes and melanoma, we note 4,128 differentially expressed genes and 56,936 differentially accessible regions with overall gene expression profiles analogous to human melanocytes and the pigmentation melanoma subtype. Combining the RNA-seq and ATAC-seq data surprisingly revealed that increased chromatin accessibility did not always correspond with increased gene expression, suggesting that though there is widespread dysregulation in chromatin accessibility in melanoma, there is a potentially more refined gene expression program driving cancerous melanoma. This data serves as a resource to identify candidate regulators of the normal vs. diseased states in a genetically controlled in vivo context.

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“…It was shown that neonatal melanocyte signatures were associated with high treatment resistance and low overall survival in melanoma patients. 3 Surprisingly, melanocyte stem cell and fetal melanocyte signatures were associated with a better prognosis, but still worse than mature melanocyte signatures. However, survival was largely based on data from treatment with immune-modulatory substances, which were not analyzed in the present study.…”

mentioning

confidence: 99%

“…These findings present in a conclusive way strong experimental evidence that oncogenic pathways must be active at a vulnerable stage of cell development to induce tumor formation, which obviously depends on the cellular context. In a recent study by Belote et al, 3 transcriptional patterns of melanocytes from different stages of development were analyzed to provide an atlas of human epidermal melanocytes. It was shown that neonatal melanocyte signatures were associated with high treatment resistance and low overall survival in melanoma patients.…”

mentioning

confidence: 99%

Melanoma development: stage-dependent cancer competence of the melanocytic lineage

Kunz¹

2021

Sig Transduct Target Ther

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Human melanocyte development and melanoma dedifferentiation at single-cell resolution

Cited by 63 publications

References 86 publications

BRAFV600E induces reversible mitotic arrest in human melanocytes via microRNA-mediated suppression of AURKB

BRAFV600E induces reversible mitotic arrest in human melanocytes via microRNA-mediated suppression of AURKB

Transcriptional profile and chromatin accessibility in zebrafish melanocytes and melanoma tumors

Melanoma development: stage-dependent cancer competence of the melanocytic lineage

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