Brad G. Hoffman; Gordon Robertson; Bogard Zavaglia; Mike Beach; Rebecca Cullum; Sam Lee; Galina Soukhatcheva; Leping Li; Elizabeth D. Wederell; Nina Thiessen; Mikhail Bilenky; Timothee Cezard; Angela Tam; Baljit Kamoh; Inanc Birol; Derek Dai; YongJun Zhao; Martin Hirst; C. Bruce Verchere; Cheryl D. Helgason; Marco A. Marra; Steven J.M. Jones; Pamela A. Hoodless

Locus co-occupancy, nucleosome positioning, and H3K4me1 regulate the functionality of FOXA2-, HNF4A-, and PDX1-bound loci in islets and liver

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Figure 6.

Site modality is independent of motif presence or score. (A) Box-whisker plots of bimodal, monomodal, or low FOXA2, PDX1, or HNF4A peak heights. Statistical significance between groups was detected using a Kruskall-Wallis non-parametric test with a Dunn's post-test, with a P < 0.05 threshold. (***) P < 0.001. (B) Fraction of peaks in the bimodal, monomodal, or low site classes in the FOXA2 (islet and liver), PDX1, HNF4A peak sets that contain a high-scoring binding motif. (C) Frequency distribution of PWM scores for the three site classes for each TF peak set.

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Published in Advance June 15, 2010, doi: 10.1101/gr.104356.109 Genome Res. 2010. 20: 1037-1051

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Locus co-occupancy, nucleosome positioning, and H3K4me1 regulate the functionality of FOXA2-, HNF4A-, and PDX1-bound loci in islets and liver

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