Physical and functional interaction of Runt-related protein 1 with hypoxia-inducible factor-1α

ZG Peng, MY Zhou, Y Huang, JH Qiu, LS Wang… - Oncogene, 2008 - nature.com
ZG Peng, MY Zhou, Y Huang, JH Qiu, LS Wang, SH Liao, S Dong, GQ Chen
Oncogene, 2008nature.com
Angiogenesis and hematopoiesis are closely linked and interactive with each other, but few
studies were given to identify possible links between angiogenesis-promoting proteins and
hematopoiesis-related transcription factors. Here we investigated the potential relationship
of oxygen-sensitive α-subunit of angiogenesis-related hypoxia-inducible factor-1α (HIF-1α)
with Runt-related protein 1 (Runx1, also known as acute myeloid leukemia-1, AML-1), an
important hematopoietic transcription factor. The results demonstrated that Runx1 and HIF …
Abstract
Angiogenesis and hematopoiesis are closely linked and interactive with each other, but few studies were given to identify possible links between angiogenesis-promoting proteins and hematopoiesis-related transcription factors. Here we investigated the potential relationship of oxygen-sensitive α-subunit of angiogenesis-related hypoxia-inducible factor-1α (HIF-1α) with Runt-related protein 1 (Runx1, also known as acute myeloid leukemia-1, AML-1), an important hematopoietic transcription factor. The results demonstrated that Runx1 and HIF-1α proteins directly interacted with each other to a degree, in which Runt homology domain of Runx1 was mainly involved. Leukemia-related abnormal Runx1 fusion protein AML1-ETO, which fuses the N-terminal 177 amino acid residues of the Runx1 protein in frame to ETO (eight-twenty-one) protein, also interacted with HIF-1α protein with greater ability than Runx1 itself. More intriguingly, Runx1 overexpression inhibited DNA-binding and transcriptional activity of HIF-1 protein with reduced expression of HIF-1-targeted genes such as vascular endothelial growth factor, while silence of Runx1 expression by specific small interfering RNA significantly increased transcriptional activity of HIF-1 protein, suggesting that Runx1 inhibited transcription-dependent function of HIF-1. Vice versa, HIF-1α increased DNA-binding ability and transcriptional activity of Runx1 protein. All these data would shed new insight to understanding Runx1 and HIF-1α-related hematopoietic cell differentiation and angiogenesis.
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