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MafG controls the hypoxic response of cells by accumulating HIF-1alpha in the nuclei.

FEBS letters (2008-06-10)
Koji Ueda, Jing Xu, Haruka Morimoto, Atsumi Kawabe, Susumu Imaoka
RESUMEN

We identified MafG as a protein that interacts with HIF-1alpha, a key factor in hypoxic response, using the yeast two-hybrid system. Interaction between MafG and HIF-1alpha was confirmed by surface plasmon resonance and by translocation to the nucleolus with the NoLS signal. A knockdown of MafG reduced erythropoietin (EPO) mRNA levels as well as luciferase reporter activity with the hypoxia response element. The knockdown of MafG did not change total HIF-1alpha protein, but reduced the accumulation of HIF-1alpha in the nuclei. These results suggest that MafG regulates the hypoxic response of cells by detaining HIF-1alpha in the nuclei.

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Anti-β-actina monoclonal antibody produced in mouse, clone AC-74, ascites fluid