FIGURE SUMMARY
Title

HMGB factors are required for posterior digit development through integrating signaling pathway activities

Authors
Itou, J., Taniguchi, N., Oishi, I., Kawakami, H., Lotz, M., and Kawakami, Y.
Source
Full text @ Dev. Dyn.

hmgb1and hmgb2 are required for enhancement of Wnt/β-catenin signaling in zebrafish embryos. Lateral views of 18-somite-stage embryos (A–E) and 36-hpf embryos (F–J) injected with control MO (A, F), hmgb1 MO (B, G), hmgb2 MO (C, H), both hmgb1 MO and hmgb2 MO (D, I) and hmgb1 MO, hmgb2 MO, Hmgb1 mRNA, and Hmgb2 mRNA (E, J). A–E: Top-GFP expression is visualized by in situ hybridization. Wnt/β-catenin signaling in forebrain (arrows), midbrain (asterisks), and tail bud (arrowhead) is visualized in control morphants (A), but downregulated in hmgb-downregulated embryos (B–D). In mRNA co-injected double morphants, Top-GFP expression is partially restored (E). Normal body extension (F) is impaired in hmgb1-morphants (G). The phenotype is less severe in hmgb2-morphants (H), but becomes more severe in double morphants (I). This phenotype was partially restored by co-injection of Hmgb1 mRNA and Hmgb2 mRNA (J).

Downregulation of Wnt signaling and shh signaling in hmgb-knockdown pectoral fin buds. Dorsal views (A–H) and lateral views (I, J) of 36-hpf embryos injected with control MO (A, C, E, G, I) or hmgb1MO + hmgb2 MO (B, D, F, H, J). A, B: Normal expression of prx1 in the pectoral fin bud of control (A, arrows) and hmgb-knockdown embryos (B, arrows). C–H: Expression of Top-GFP (D), shh (F), and ptc1 (H) in the pectoral fin bud of hmgb-knockdown embryos (D, F, H, red arrows) is downregulated, compared to control embryos (C, E, G, black arrows). I, J: High-magnification images of the pectoral fin bud stained with shh shows smaller expression domain of shh in the pectoral fin bud of hmgb-knockdown embryos (J, red arrow), compared to the control fin bud (I, black arrow).

Acknowledgments
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