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sox2xenopus   

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Experiment details for sox2

Khokha MK et al. (2005) Assay

Depletion of three BMP antagonists from Spemann's organizer leads to a catastrophic loss of dorsal structures.

Gene Clone Species Stages Anatomy
sox2 tropicalis NF stage 14 to NF stage 15 pre-chordal neural plate , chordal neural plate , neural plate

  Figure 2. Single Morphants and Double Morphants Still Form a Substantial Neural PlateAll panels show sox2 expression to visualize the neural plate (dorsal views with anterior to the bottom) in neurula embryos (st 14–15). Uninjected embryos are shown (A, D, and G) with sibling noggin morphants (B), follistatin morphants (E), and chordin morphants (H). Double morphants include follistatin/noggin (K), chordin/noggin (N), and chordin/follistatin (Q) and are shown with sibling uninjected embryos (J, M, and P). Morphants were rescued with pufferfish noggin (C, F, I, L, O, and R). Abbreviations are as follows: F = follistatin, C = chordin, N = noggin, UC = uninjected sibling control embryos, MO = morphant, and MO + R = morphant rescued with noggin mRNA.

Gene Clone Species Stages Anatomy
sox2 tropicalis NF stage 14 to NF stage 15 neural plate

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  Figure 3. FCN Morphants Have a Catastrophic Loss in Dorsal DevelopmentAll panels are dorsal views with anterior to the top of st 14–15 neurula embryos. Expression of multiple dorsal markers (sox2 [A–D], sox3 [E–H], myf5 [I–L], myoD [M–P], shh [Q–T], and xnot [U–X]) are shown in uninjected sibling embryos (A, C, E, G, I, K, M, O, Q, S, U, and W) and follistatin, chordin, and noggin (FCN) triple morphants (B, F, J, N, R, and V) as well as β-catenin morphants (D, H, L, P, T, and X) for comparison.

Gene Clone Species Stages Anatomy
sox2 tropicalis NF stage 14 neural plate

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  Figure 4. The Phenotype of the FCN Triple Morphant Is Specific to a Loss in BMP AntagonismAll panels are dorsal views of neurula embryos (st 14) with anterior to the top. Triple morphants were subsequently injected with pufferfish noggin mRNA (C, F, and I) and show substantial rescue of dorsal structures (sox2 [A–C], myoD [D–F], and shh [G–I]) when compared to triple morphants (B, E, and H) and uninjected sibling embryos (A, D, and G). The distribution of phenotypes seen in these rescue experiments is depicted in a bar graph (J). The vertical axis is the percent of embryos that show a particular phenotype. The horizontal axis shows the experimental groups and the phenotypes seen. The black bar depicts the percentage of embryos with a substantial neural plate, the dark gray bar depicts the percentage of embryos with a minor neural plate, and the light gray bar depicts the percentage of embryos with no neural plate that show only a ring of sox2 expression. We also tested the phenotype of the triple morphant for specificity by subsequently injecting BMP4,7 MOs (BMP MO), which should reduce BMP signaling. A partial rescue of the neural plate is seen (M) compared to triple morphants (L) and uninjected sibling control embryos (K).