2009
DOI: 10.1073/pnas.0811186106
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Genetic evidence for shared mechanisms of epimorphic regeneration in zebrafish

Abstract: In a microarray-based gene profiling analysis of Mü ller glia-derived retinal stem cells in light-damaged retinas from adult zebrafish, we found that 2 genes required for regeneration of fin and heart tissues in zebrafish, hspd1 (heat shock 60-kDa protein 1) and mps1 (monopolar spindle 1), were up-regulated. Expression of both genes in the neurogenic Mü ller glia and progenitors was independently verified by quantitative reverse transcriptase PCR and in situ hybridization. Functional analysis of temperature-se… Show more

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Cited by 129 publications
(176 citation statements)
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References 39 publications
(54 reference statements)
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“…Increase of msxb expression is required for tissue outgrowth during regeneration (Thummel et al, 2010). Genetic control of organ regeneration has been reported in other zebrafish organs, such as heart, spinal cord, and retina (Curado et al, 2007;Schoenebeck et al, 2007;Qin et al, 2009;Jopling et al, 2010;Montgomery et al, 2010).…”
Section: Discussionmentioning
confidence: 99%
See 1 more Smart Citation
“…Increase of msxb expression is required for tissue outgrowth during regeneration (Thummel et al, 2010). Genetic control of organ regeneration has been reported in other zebrafish organs, such as heart, spinal cord, and retina (Curado et al, 2007;Schoenebeck et al, 2007;Qin et al, 2009;Jopling et al, 2010;Montgomery et al, 2010).…”
Section: Discussionmentioning
confidence: 99%
“…While amphibians have long been the central characters employed in studies on tissue or organ regeneration (Brockes, 1997;Beck et al, 2009;Contreras et al, 2009;Kragl et al, 2009;Calve et al, 2010), the zebrafish (Danio rerio) have recently emerged as a new vertebrate model for genetic studies of tissue/ organ regeneration. Like amphibians, zebrafish exhibit an enhanced capability of regenerating adult tissues, which include retina, spinal cord, kidney, heart, and fin (Poss et al, 2000a(Poss et al, ,b, 2002aNechiporuk and Keating, 2002;Nechiporuk et al, 2003;Jazwinska et al, 2007;Schoenebeck et al, 2007;Tsai et al, 2007;Qin et al, 2009;Jopling et al, 2010;Thummel et al, 2010). Fin regeneration is a particularly efficient model for studying tissue regeneration.…”
Section: Introductionmentioning
confidence: 99%
“…28 For photoreceptors in the outer nuclear layer, the Zpr1 antibody labels a cell surface epitope on red/green-sensitive double cones and the Zpr3 antibody labels an antigenic region on the rods. [29][30][31] At 72 hpf, the ganglion cell layer, inner nuclear layer, and outer nuclear layer were fully laminated. Meanwhile, ganglion cells, cones, and rods were well-differentiated in the retinas of the unexposed group (Figure 5A-C).…”
Section: Neuronal Differentiation Was Delayed Following Cuo Nps Exposurementioning
confidence: 99%
“…Dedifferentiation is thought to occur, for example, during regeneration of the teleost retina by Müller glia cells that share several morphological and molecular properties with RG Bernardos et al, 2007;Ganz et al, 2010;Hitchcock and Raymond, 2004;Qin et al, 2009;Stenkamp, 2007;Thummel et al, 2008), but also in axolotl limb regeneration (Kragl et al, 2009) and during zebrafish bone regeneration (Knopf et al, 2011). For adult RG, the answer probably requires a more rigorous understanding of dedifferentiation.…”
Section: Dedifferentiation Of Radial Glia?mentioning
confidence: 99%