Journal
BIOSCIENCE REPORTS
Volume 34, Issue -, Pages 765-774Publisher
PORTLAND PRESS LTD
DOI: 10.1042/BSR20140116
Keywords
AML; oestrogen receptor; gene regulation; HOXA10; mixed lineage leukaemia
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Funding
- National Nature Scientific Foundation of China [81000225]
- Natural Science Foundation Project of CQ CSTC [CSTC2013jcyja0102]
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HOXA10, a homeobox-containing gene involved in definitive haematopoiesis, which implicated in the pathogenesis of AML (acute myeloid leukaemia), has been studied extensively. But the regulatory mechanism that drives HOXA10 expression is still unclear. In the present paper, HOXA10 regulated by MLL1 (mixed lineage leukaemia histone methylase 1) with an epigenetic way has been demonstrated. The HOXA10 promoter contains several EREs (oestrogen response elements), including ERE1 and ERE2, which are close to the transcription start site, and are associated with E2-mediated activation of HOXA10. It has been shown that knockdown of the ER alpha (oestrogen receptor alpha) suppresses E2-mediated activation of HOXA10. Similarly, knockdown of MLL1 suppresses activation of HOXA10 and is bound to the ERE of HOXA10 promoter in an E2-dependent manner by forming complex with ER alpha. Knockdown of ER alpha affects the E2-dependent binding of MLL1 into HOXA10 EREs, suggesting critical roles of ER alpha in recruiting MLL on the HOXA10 promoter. More interestingly, the methylation status of histone protein H3K4 (H3 at lysine 4) with E2 is much higher than without E2 treatment in leukaemia cell. On the contrary, the methylation status of HOXA10 promoter with E2 treatment is much lower, which elevate the HOXA10 expression. Moreover, with ER alpha knockdown, the H3K4 methylation level is also decrease in myeloid cell. Overall, it has been clearly demonstrated that HOXA10 is transcriptionally regulated by MLL1, which, in coordination with ERa, plays a critical role in this process with epigenetic way and suggests a potential anti-E2 treatment of AML.
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