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Hypoxia-induced HIF1? targets in melanocytes reveal a molecular profile associated with poor melanoma prognosis.


ABSTRACT: Hypoxia and HIF1? signaling direct tissue-specific gene responses regulating tumor progression, invasion, and metastasis. By integrating HIF1? knockdown and hypoxia-induced gene expression changes, this study identifies a melanocyte-specific, HIF1?-dependent/hypoxia-responsive gene expression signature. Integration of these gene expression changes with HIF1? ChIP-Seq analysis identifies 81 HIF1? direct target genes in melanocytes. The expression levels for 10 of the HIF1? direct targets - GAPDH, PKM, PPAT, DARS, DTWD1, SEH1L, ZNF292, RLF, AGTRAP, and GPC6 - are significantly correlated with reduced time of disease-free status in melanoma by logistic regression (P-value = 0.0013) and ROC curve analysis (AUC = 0.826, P-value < 0.0001). This HIF1?-regulated profile defines a melanocyte-specific response under hypoxia, and demonstrates the role of HIF1? as an invasive cell state gatekeeper in regulating cellular metabolism, chromatin and transcriptional regulation, vascularization, and invasion.

SUBMITTER: Loftus SK 

PROVIDER: S-EPMC5411287 | biostudies-literature | 2017 May

REPOSITORIES: biostudies-literature

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Hypoxia-induced HIF1α targets in melanocytes reveal a molecular profile associated with poor melanoma prognosis.

Loftus Stacie K SK   Baxter Laura L LL   Cronin Julia C JC   Fufa Temesgen D TD   Pavan William J WJ  

Pigment cell & melanoma research 20170419 3


Hypoxia and HIF1α signaling direct tissue-specific gene responses regulating tumor progression, invasion, and metastasis. By integrating HIF1α knockdown and hypoxia-induced gene expression changes, this study identifies a melanocyte-specific, HIF1α-dependent/hypoxia-responsive gene expression signature. Integration of these gene expression changes with HIF1α ChIP-Seq analysis identifies 81 HIF1α direct target genes in melanocytes. The expression levels for 10 of the HIF1α direct targets - GAPDH,  ...[more]

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