Identification of a ZEB2-MITF-ZEB1 transcriptional network that controls melanogenesis and melanoma progression

Deregulation of signaling pathways that control differentiation, expansion and migration of neural crest-derived melanoblasts during normal development contributes also to melanoma progression and metastasis. Although several epithelial-to-mesenchymal (EMT) transcription factors, such as zinc finger...

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Veröffentlicht in:Cell Death and Differentiation 2014-08, Vol.21 (8), p.1250-1261
Hauptverfasser: Denecker, G, Vandamme, Nele, Akay, O, Koludrovic, D, Taminau, J, Lemeire, K, Gheldof, A, De Craene, B, Van Gele, M, Brochez, L, Udupi, G.M, Rafferty, M, Balint, B, Gallagher, W.M, Ghanem, G, Huylebroeck, Danny, Haigh, J, van den Oord, Joost, Larue, L, Davidson, I, Marine, Chris, Berx, G
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container_end_page 1261
container_issue 8
container_start_page 1250
container_title Cell Death and Differentiation
container_volume 21
creator Denecker, G
Vandamme, Nele
Akay, O
Koludrovic, D
Taminau, J
Lemeire, K
Gheldof, A
De Craene, B
Van Gele, M
Brochez, L
Udupi, G.M
Rafferty, M
Balint, B
Gallagher, W.M
Ghanem, G
Huylebroeck, Danny
Haigh, J
van den Oord, Joost
Larue, L
Davidson, I
Marine, Chris
Berx, G
description Deregulation of signaling pathways that control differentiation, expansion and migration of neural crest-derived melanoblasts during normal development contributes also to melanoma progression and metastasis. Although several epithelial-to-mesenchymal (EMT) transcription factors, such as zinc finger E-box binding protein 1 (ZEB1) and ZEB2, have been implicated in neural crest cell biology, little is known about their role in melanocyte homeostasis and melanoma. Here we show that mice lacking Zeb2 in the melanocyte lineage exhibit a melanoblast migration defect and, unexpectedly, a severe melanocyte differentiation defect. Loss of Zeb2 in the melanocyte lineage results in a downregulation of the Microphthalmia-associated transcription factor (Mitf) and melanocyte differentiation markers concomitant with an upregulation of Zeb1. We identify a transcriptional signaling network in which the EMT transcription factor ZEB2 regulates MITF levels to control melanocyte differentiation. Moreover, our data are also relevant for human melanomagenesis as loss of ZEB2 expression is associated with reduced patient survival.
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title Identification of a ZEB2-MITF-ZEB1 transcriptional network that controls melanogenesis and melanoma progression
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