RNA-seq analysis identifies different transcriptomic types and developmental trajectories of primary melanomas

Kunz, Manfred; Löffler-Wirth, Henry; Dannemann, Michael; Willscher, Edith; Doose, Gero; Kelso, Janet; Kottek, Tina; Nickel, Birgit; Hopp, Lydia; Landsberg, Jenny; Hoffmann, Steve; Tüting, Thomas; Zigrino, Paola; Mauch, Cornelia; Utikal, Jochen; Ziemer, Mirjana; Schulze, Hans‐Joachim; Hölzel, Michael; Roesch, Alexander; Kneitz, Susanne; Meierjohann, Svenja; Boßerhoff, Anja; Binder, Hans; Schartl, Manfred

doi:10.1038/s41388-018-0385-y

Cited by 84 publications

(93 citation statements)

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“…We assigned all genes within these regions to the respective state and further processed them in analogy to gene sets that provided GSZ-values for each sample [see also Ref. ( 29 ) for details]. Heatmap presentations were generated by standard R-functions including hierarchical clustering options.…”

Section: Methodsmentioning

confidence: 99%

Footprints of Sepsis Framed Within Community Acquired Pneumonia in the Blood Transcriptome

et al. 2018

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We analyzed the blood transcriptome of sepsis framed within community-acquired pneumonia (CAP) and characterized its molecular and cellular heterogeneity in terms of functional modules of co-regulated genes with impact for the underlying pathophysiological mechanisms. Our results showed that CAP severity is associated with immune suppression owing to T-cell exhaustion and HLA and chemokine receptor deactivation, endotoxin tolerance, macrophage polarization, and metabolic conversion from oxidative phosphorylation to glycolysis. We also found footprints of host’s response to viruses and bacteria, altered levels of mRNA from erythrocytes and platelets indicating coagulopathy that parallel severity of sepsis and survival. Finally, our data demonstrated chromatin re-modeling associated with extensive transcriptional deregulation of chromatin modifying enzymes, which suggests the extensive changes of DNA methylation with potential impact for marker selection and functional characterization. Based on the molecular footprints identified, we propose a novel stratification of CAP cases into six groups differing in the transcriptomic scores of CAP severity, interferon response, and erythrocyte mRNA expression with impact for prognosis. Our analysis increases the resolution of transcriptomic footprints of CAP and reveals opportunities for selecting sets of transcriptomic markers with impact for translation of omics research in terms of patient stratification schemes and sets of signature genes.

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Section: Methodsmentioning

confidence: 99%

Footprints of Sepsis Framed Within Community Acquired Pneumonia in the Blood Transcriptome

et al. 2018

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“…Thus, to analyze pri-miR-29 expression during melanomagenesis we performed RNA sequencing on four wildtype BRAF human melanocyte cell lines (Hermes1, Hermes2, Hermes3A, and Hermes4B) and five human melanoma cell lines (WM35, 1205Lu, WM164, SKMel28 and WM793) harboring the oncogenic BRAF V600E mutation. In addition, we interrogated pri-miR-29 expression in a publicly available RNAseq dataset (Kunz et al 2018) containing 23 nevi and 57 primary melanomas. In agreement with our observations, we found that there was a trend towards increased pri-miR-29b1~a expression in melanoma cell lines and primary melanomas compared to melanocyte cell lines and nevi, respectively ( Figure 3E and 3F).…”

Section: The Mapk Pathway Regulates Mir-29 Expression In Human Melanomentioning

confidence: 99%

MAPK-induced miR-29 targets MAFG and suppresses melanoma development

Vera

Bok

Jasani

et al. 2020

Preprint

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The tumor suppressive miR-29 family of microRNAs is encoded by two clusters, miR-29b1~a and miR-29b2~c, and is regulated by several oncogenic and tumor suppressive stimuli. Here we investigated whether oncogenic MAPK hyperactivation regulates miR-29 abundance and how this signaling axis impacts melanoma development. Using mouse embryonic fibroblasts and human melanocytes, we found that oncogenic MAPK signaling stimulates p53-independent and p53-dependent transcription of pri-miR-29b1~a and pri-miR-29b2~c, respectively. Expression analyses revealed that while pri-miR-29a~b1 remains elevated, pri-miR-29b2~c levels decrease during melanoma progression. Using a rapid mouse modeling platform, we showed that inactivation of miR-29 in vivo accelerates the development of frank melanomas and decreases overall survival. We identified MAFG as a relevant miR-29 target that has oncogenic potential in melanocytes and is required for growth of melanoma cells. Our findings suggest that MAPK-driven miR-29 induction constitutes a tumor suppressive barrier by targeting MAFG, which is overcome by attenuation of miR-29b2~c expression.

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“…It is thought that bypass from a senescence program contributes to the malignant transformation of benign nevi, but the mechanism of this process remains only partly understood. Recently, gene expression profiling of benign nevi and melanomas characterized two transcriptomic types of melanocytic nevi and primary melanomas (Kunz et al, 2018). The two melanoma subtypes were associated with a high versus low rate of NRAS mutation and harbored gene expression signatures for BRAF/MEK and anti-PD-1 treatment resistance, respectively.…”

Section: Genomic Analysis Of Metastatic Melanoma In An Adult With Giamentioning

confidence: 99%

Genomic analysis of metastatic melanoma in an adult with giant congenital melanocytic nevus

Chang

Iqbal

Badal

et al. 2020

Pigment Cell Melanoma Res

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RNA-seq analysis identifies different transcriptomic types and developmental trajectories of primary melanomas

Cited by 84 publications

References 50 publications

Footprints of Sepsis Framed Within Community Acquired Pneumonia in the Blood Transcriptome

Footprints of Sepsis Framed Within Community Acquired Pneumonia in the Blood Transcriptome

MAPK-induced miR-29 targets MAFG and suppresses melanoma development

Genomic analysis of metastatic melanoma in an adult with giant congenital melanocytic nevus

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