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	Figure 1. Effect of pifithrin-α on limb regeneration. (A & E) Controls treated daily with DMSO. (B-D & F-G) Pifithrin-α treated animals (5 μM pifithrin-α, added freshly diluted everyday). Limbs in panels A-D were amputated distally in the middle of the zeugopod and limbs in panels E-G were amputated proximally through the middle of the stylopod (see dotted lines in panels A & E for amputation levels).
	Figure 2. Comparison between Human and axolotl p53 important domains, regions and residues. (A) Schematic structure of p53 protein (adapted from Appella, 2001 [71]): TA, Transactivation Domain; DBD, DNA Binding Domain; NLS, Nuclear Localisation Signal; TET, tetramerisation domain; REG, Regulatory domain; Regions I-V, highly conserved regions. Lysine (K), serine (S) and threonine (T) residues implicated in post-translational modifications are indicated. The protein domains depicted in the diagrams are not to scale. (B) Sequences alignment of human and axolotl p53 proteins. The conserved regions I to V are highlighted and many changes between the axolotl and human sequence are identified (arrows). See table-2 for a complete list of changes associated with mutations in the human protein.
	Figure 3. Phylogenetic tree of p53 protein sequences in vertebrates with bootstrap values. Maximum likelihood phylogenetic tree based on 35 p53 sequences with 280 amino acid positions inferred by the program Treefinder with a WAG+Γ8 model. Numbers at internal nodes are corresponding to bootstrap support values, obtained in the analysis of 100 replicates using the same program and model of sequence evolution. Due to the dense species sampling within the mammals interesting aspects of mammalian evolution are becoming apparent. There are clear differences in the evolutionary rates among the different groups, indicated by the branch length of the rooted tree, this is especially true for the four Neoteleost fish. There is also an acceleration observed for the mouse-like rodents, with a striking exception represented by the sequence of the mole rat Spalax, which is despite the fact of being a rather small rodent even more slowly evolving than the related rabbit (Oryctolagus, lagomorph). In fact the only sequences among the tetrapods (amphibians, reptilian and mammalian) that are more slowly evolving than the one from Spalax are from the urodeles (axolotl and newts). The primary sequence of salamander p53 is more closely related to the ancestral protein of tetrapod vertebrates than the p53 proteins of any other of the studied groups.
	Figure 4. Activation of Hdm2 and p21 promoters by human and axolotl p53 in H1299 cells. (A-C) Dual-luciferase assays in H1299 cells with Hdm2 promoter at 37°C, 30°C and 25°C. (D-F) Dual-luciferase assays in H1299 cells with the human p21 promoter at 37°C, 30°C and 25°C. Luciferase activities stimulated by human or axolotl p53 was significantly different than non-p53 controls (at least p < 0.05, data not shown). Error bars are ± s.e.m. human and axolotl p53 luciferase transactivation were significantly different during the same assay using the Hdm2 promoter (A-C) or the human p21 promoter at 37°C (D) (at least p < 0.01). Each assay was performed in triplicate at least 3 separate times. (G) Inhibition of the activation of Hdm2 promoter by the combined expression of human and axolotl p53 in H1299 cells. All luciferase activities were significantly different than non-p53 controls (at least p < 0.05, data not shown). Error bars are ± s.e.m. human + axolotl and human p53 luciferase transactivation were significantly different during the same assay using the Hdm2 promoter at 37°C (p = 0.006). Each assay was performed in triplicate. (H) Growth assays at 37°C on H1299 cells transfected with human or axolotl p53 protein.
	Figure 5. Activation of endogenous Hdm2 in H1299 cells by the axolotl p53 protein. Expression of the human p53 target gene (Hdm2) 24 h post transfection in H1299 cells mock transfected and transfected with the axolotl p53 without and with pifithrin-α grown at 30°C. RT-PCRs were also performed with the housekeeping gene glyceraldehyde phosphate dehydrogenase (Gapdh) to control for the amount of total RNA.
	Figure 6. Activation of Hdm2 and p21 promoters by human and axolotl p53 in AL1 cells. (A-B) Dual-luciferase assays in AL1 cells with Hdm2 and p21 promoters at 25°C. All Luciferase activities were significantly different from non-p53 controls (at least p < 0.05, data not shown). Error bar ± s.e.m. human and axolotl p53 induced luciferase expression were significantly different with the Hdm2 promoter (p < 0.01). Each assay was performed in triplicate at least 3 separate times.
	Figure 7. Detection of p53 protein in AL1 cells. (A & C) Western blot analysis of phospho-ser15 p53 in AL1 cells exposed to UV or treated with MNNG. (B) RT-PCR analysis of p53 target gene, Gadd45 (a p53 target gene cloned in axolotl [57, 58]), in control treated axolotl AL1 cells, cells exposed to UV (6h post-irradiation) and cells exposed to UV & treated with pifithrin-α. Both Gapdh and Ef1α were used as controls to demonstrate that the effects of UV and UV plus pifithrin-α were specific for Gadd45. (D-E) Western blot analysis of total p53 protein (CM5 antibody) on AL1 cells exposed to UV or treated with MNNG.

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