Mescher AL et al. (2013), Changes in the inflammatory response to injury ...

XB-ART-47753

PLoS One 2013 Jan 01;811:e80477. doi: 10.1371/journal.pone.0080477.

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Changes in the inflammatory response to injury and its resolution during the loss of regenerative capacity in developing Xenopus limbs.

Mescher AL , Neff AW , King MW .

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Tissue and organ regeneration, unlike development, involves an injury that in postembryonic animals triggers inflammation followed by resolution. How inflammation affects epimorphic regeneration is largely uninvestigated. Here we examine inflammation and its resolution in Xenopus laevis hindlimb regeneration, which declines during larval development. During the first 5 days postamputation, both regeneration-competent stage 53 and regeneration-deficient stage 57 hindlimbs showed very rapid accumulation of leukocytes and cells expressing interleukin-1β and matrix metalloproteinase 9. Expression of genes for factors mediating inflammatory resolution appeared more persistent at stages 55 and 57 than at stage 53, suggesting changes in this process during development. FoxP3, a marker for regulatory T cells, was upregulated by amputation in limbs at all three stages but only persisted at stage 57, when it was also detected before amputation. Expression of genes for cellular reprogramming, such as SALL4, was upregulated in limbs at all 3 stages, but markers of limb patterning, such as Shh, were expressed later and less actively after amputation in regeneration-deficient limbs. Topical application of specific proinflammatory agents to freshly amputated limbs increased interleukin-1β expression locally. With aqueous solutions of the proinflammatory metal beryllium sulfate, this effect persisted through 7 days postamputation and was accompanied by inhibition of regeneration. In BeSO4-treated limbs expression of markers for both inflammation and resolution, including FoxP3, was prolonged, while genes for cellular reprogramming were relatively unaffected and those for limb patterning failed to be expressed normally. These data imply that in Xenopus hindlimbs postamputation inflammation and its resolution change during development, with little effect on cellular dedifferentiation or reprogramming, but potentially interfering with the expression of genes required for blastema patterning. The results suggest that developmental changes in the larval anuran immune system may be involved in the ontogenetic loss of epimorphic regeneration in this system.

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Species referenced: Xenopus laevis
Genes referenced: anxa1 fga fgl2 foxp3 hoxa13 hpse il1b lgals1.1 mpo msx1 odc1 sall1 sall4 shh socs1 socs3 tbx3

Phenotypes: Xla Wt + BeSO4 + hindlimb amputation (a) [+]

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	Figure 1. Whole-mounts of stage 53 and stage 57 Xenopus hindlimbs from 0 hours to 5 days post-amputation (PA) stained by enzyme histochemistry for myeloperoxidase (MPO), a marker for neutrophils and macrophages. Only background staining is visible at the time of amputation (0 hPA), but by 6 hPA in limbs of both stages the number of brown MPO+ cells increase greatly near the site of amputation. MPO staining diminished slowly through 5 dPA in limbs of both stages. The larger, very dark structures are melanocytes.
	Figure 2. Expression of genes previously identified in studies of gene activity during the early phase of Xenopus limb regeneration, shown by RT-PCR at different times PA during the transition from regeneration-complete to incomplete in stages 53, 55, and 57. Tissue from 20 limb stumps was used for each time point and expression of the loading control ornithine decarboxylase (ODC) is shown in the top row. (a) Genes with primarily inflammation-related function: Expression of interleukin-1β (IL-1β) appeared maximal by 6 hPA but then was rapidly diminished at all stages. Expression of factors involved in the resolution of inflammation, including annexin-A1 (ANXA1), fibrinogen-like protein 2 (FGL2), suppressors of cytokine signaling (SOCS) 1 and 3, galectin-1, and the key marker for regulatory T cells, FoxP3, were also all up-regulated by 6hPA and then diminished in limbs of all 3 stages, but more slowly in regeneration-incomplete limbs suggesting that inflammation-related activity persists after amputation in the more developed limbs. Low expression of many of these pro-resolution factors, including FoxP3, was seen already at the time of amputation in regeneration-deficient limbs, indicating the presence of immune cells not found in limbs at early regeneration-complete stages. (b) Genes with primarily cell reprogramming and organ patterning function: Expression of SALL4 and TBX3, both involved in cell reprogramming during early blastema formation, are up-regulated by amputation at all 3 stages, but much more slowly and at apparently lower levels in regeneration-incomplete limbs. Expression of genes required for blastema patterning, including Shh, Msx1, SALL1, and HOXA13, occurred at various times PA in stage 53 limbs, but was increasingly reduced and delayed in regeneration-deficient limbs, results consistent with the failure of the latter limbs to regenerate with normal patterns. Cycle number for ODC PCR was 25; FoxP3 required 40 cycles and all other genes 30.

	Figure 5. Expression of genes in control and 104-treated stage 53 limbs in vivo and in organ culture at various times after amputation. show more Although ornithine decarboxylase (ODC) expression (top) is reduced uniformly by explantation, possibly due to decreased cell viability, clear differences in expression of other genes are observed between limb stumps in vivo and in vitro. (a) Expression of the inflammation-related genes IL-1β, FGL-2, MMP-9, complement C3 and C4, and of FoxP3+ regulatory T cells, all appear to be up-regulated in Be-treated limb stumps compared to untreated controls. For all these genes except C3 and C4 expression was not seen or was reduced (FoxP3) in explanted limb stumps, indicating that in vivo this gene expression occurs in immigrating leukocytes. (b) In contrast, expression of genes forSALL4 (which was not inhibited by Be treatment) and limb patterning genes was detected in explanted as well as intact limbs. *FoxP3 PCR required 40 cycles; ODC PCR was carried out for 25 cycles and all other genes were assayed with 30 cycles.
	Figure 4. Quantitative PCR of gene expression through 7 days post-amputation in control and 10 mM BeSO4-treated stage 53/54 limbs.Tissue from 20 limb stumps was used for each time point. (Top) In untreated control limbs expression of inflammation-related IL-1β and FGL-2 are transient, expression of the patterning genes Shh and SALL1 begins by 3 dPA, and expression of the reprogramming gene SALL4 occurs throughout this period. In Be-treated limb stumps, IL-1β expression persists through 7 dPA, expression of the proresolution factor FGL-2 is five-fold higher than in controls and also highly persistent, while SALL4 and TBX3 expression is similar to that of control regenerates and expression of SALL1 and Shh remains very low. (Bottom) Compared individually expression of proinflammatory IL-1β and proresolution FGL-2 are both significantly elevated and persistent through 7 dPA in Be-treated limbs. In general Be had no significant effect on expression of SALL4, but inhibited expression of the patterning-related genesTBX3, SALL1 and Shh. Each time point shows the mean of triplicate PCR runs, with standard deviations. Statistical comparisons are between similar time points in the treated and untreated groups: * = P<0.05, ** = P<0.001, and no symbol indicating no statistical differences.

References [+] :

Ariel, Hanging in the balance: endogenous anti-inflammatory mechanisms in tissue repair and fibrosis. 2013, Pubmed