Hypoxia-related Transcription factor ChIP-Seq data in T47D breast cancer cells

We report the comprehensive genome-wide binding peaks for key factors inovled in oxygen sensing pathways, such as HIF1a, HIF1ß and EglN2. In addition, we also report the genome-wide binding peaks for NRF1 in breast cancer cells Overall design: We conducted HA-EglN2, HIF1a, HIF1ß (ARNT) or NRF1 ChIP-Seq in the T47D cell line that overexpresses HA-EglN2 in the presence of hypoxia (1%) and DMOG treatment. T47D parental cells treated with the same condition followed by HA ChIP-seq served as the control to filter non-specific binding.