FIGURE

Fig. 4

ID
ZDB-FIG-120423-25
Publication
Arkhipova et al., 2012 - Characterization and regulation of the hb9/mnx1 beta-cell progenitor specific enhancer in zebrafish
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Fig. 4

In vitro binding of NeuroD and Pax6b to PE specific sequence motives. (A) Schematic representation of potential binding sites for the transcription factors NeuroD (E-box in red) and Pax6 (blue) within the hb9 pancreas enhancer as revealed by bioinformatic sequence analyses. Pax6 sites with a core match between 0.76 and 0.9 are shown in light blue, and sites with a core match between 0.9 and 1 are shown in dark blue (core = TCACG). Orientation of Pax6 sites is indicated by position relative to the line (above: positive DNA strand; below: negative DNA). (B) EMSA studies show binding of in vitro synthesized NeuroD/E47 dimers (Prot) to oligonucleotides (DNA) spanning the E-boxes (E1, E2) but not to corresponding oligonucleotides with mutated E boxes (E1m and E2m). Competitor assays with unlabelled oligonucleotides (comp, as indicated) revealed efficient competition by E1 and E2 but not by E1m and E2m. Notably, unlabelled E2m reduced binding of labelled E2 to NeuroD/E47, suggesting that E2 binds NeuroD/E47 with lower affinity as compared to E1. Bands indicated by the asterisk presumably correspond to monomeric DNA–protein complexes. (C) EMSA studies with in vitro synthesized Pax6b protein (Prot) and oligonucleotides spanning individual or multiple potential Pax6b sites (as indicated). EMSA signals could be detected for P1 + 2 + 3, P4 + 5 + 6, P7 + 8, P9 + 10, P14 but not for P11, P12 and P13 (positions of protein-bound DNAs are indicated by arrowhead).

Expression Data

Expression Detail
Antibody Labeling
Phenotype Data

Phenotype Detail
Acknowledgments
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Reprinted from Developmental Biology, 365(1), Arkhipova, V., Wendik, B., Devos, N., Ek, O., Peers, B., and Meyer, D., Characterization and regulation of the hb9/mnx1 beta-cell progenitor specific enhancer in zebrafish, 290-302, Copyright (2012) with permission from Elsevier. Full text @ Dev. Biol.