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Global transcriptional analysis identifies a novel role for SOX4 in 2 tumor-induced angiogenesis

Authors :
Vervoort, SJ
De Jong, OG
Roukens, MG
Frederiks, CL
Vermeulen, JF
Lourenço, AR
Bella, L
Vidakovic, AT
Sandoval, JL
Moelans, C
Van Amersfoort, M
Dallman, MJ
Bruna, A
Caldas, C
Nieuwenhuis, E
Van der Wall, E
Derksen, P
Van Diest, P
Verhaar, MC
Lam, EW-F
Mokry, M
Coffer, PJ
Cancer Research UK
Breast Cancer Now
Medical Research Council (MRC)
Publication Year :
2018
Publisher :
eLife Sciences Publications Ltd, 2018.

Abstract

The expression of the transcription factor SOX4 is increased in many human cancers, however, the pro-oncogenic capacity of SOX4 can vary greatly depending on the type of tumor. Both the contextual nature and the mechanisms underlying the pro-oncogenic SOX4 response remain unexplored. Here, we demonstrate that in mammary tumorigenesis, the SOX4 transcriptional network is dictated by the epigenome and is enriched for pro-angiogenic processes. We show that SOX4 directly regulates endothelin-1 (ET-1) expression and can thereby promote tumor-induced angiogenesis both in vitro and in vivo. Furthermore, in breast tumors, SOX4 expression correlates with blood vessel density and size, and predicts poor-prognosis in patients with breast cancer. Our data provide novel mechanistic insights into context-dependent SOX4 target gene selection, and uncover a novel pro-oncogenic role for this transcription factor in promoting tumor-induced angiogenesis. These findings establish a key role for SOX4 in promoting metastasis through exploiting diverse pro-tumorigenic pathways.

Details

Database :
OpenAIRE
Accession number :
edsair.od......1032..b9f412bb65c8fbe503270d8426f34c10