Michael R. Tallack; Tom Whitington; Wai Shan Yuen; Elanor N. Wainwright; Janelle R. Keys; Brooke B. Gardiner; Ehsan Nourbakhsh; Nicole Cloonan; Sean M. Grimmond; Timothy L. Bailey; Andrew C. Perkins

A global role for KLF1 in erythropoiesis revealed by ChIP-seq in primary erythroid cells

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Figure 6.

Analysis of KLF1- and GATA1-bound genomic regions reveals potential interacting transcription factor partners. A schematic representation of the overlap between KLF1, GATA1 (Cheng et al. 2009) and SCL (Wilson et al. 2009) erythroid ChIP-seq datasets defines two major groups of KLF1 binding sites, total binding sites (945), and shared KLF1-GATA1 binding sites (397). Interrogation of binding site sequences using the Clover algorithm identifies the motifs shown as being overrepresented in the groups shown at 0.05 and 0.1 P-value significance levels.

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Published in Advance May 27, 2010, doi: 10.1101/gr.106575.110 Genome Res. 2010. 20: 1052-1063

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A global role for KLF1 in erythropoiesis revealed by ChIP-seq in primary erythroid cells

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