An RNAi Screen Reveals Intestinal Regulators of Branching Morphogenesis, Differentiation, and Stem Cell Proliferation in Planarians

Forsthoefel, David J.; James, Noelle; Escobar, David; Stary, Joel M.; Vieira, Ana Paula; Waters, Forrest A.; Newmark, Phillip A.

doi:10.1016/j.devcel.2012.09.008

Cited by 120 publications

(147 citation statements)

References 97 publications

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“…mitfl-1 was primarily detected in differentiated intestinal cells (supplementary material Fig. S2), and gene knockdown caused severe regeneration abnormalities and dorsal lesions that resulted in death, a phenotype reminiscent of defects observed after the loss of intestinal integrity (Forsthoefel et al, 2012). Consistent with previous reports, gene silencing of tfc15 (Wagner et al, 2011) resulted in no discernible phenotype, whereas myoD RNAi caused regeneration blastema patterning defects (Reddien et al, 2005a).…”

Section: Analysis Of Bhlh Gene Function In Cns Regenerationsupporting

confidence: 76%

Genome-wide analysis of the bHLH gene family in planarians identifies factors required for adult neurogenesis and neuronal regeneration

et al. 2013

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In contrast to most well-studied model organisms, planarians have a remarkable ability to completely regenerate a functional nervous system from a pluripotent stem cell population. Thus, planarians provide a powerful model to identify genes required for adult neurogenesis in vivo. We analyzed the basic helix-loop-helix (bHLH) family of transcription factors, many of which are crucial for nervous system development and have been implicated in human diseases. However, their potential roles in adult neurogenesis or central nervous system (CNS) function are not well understood. We identified 44 planarian bHLH homologs, determined their patterns of expression in the animal and assessed their functions using RNAi. We found nine bHLHs expressed in stem cells and neurons that are required for CNS regeneration. Our analyses revealed that homologs of coe, hes (hesl-3) and sim label progenitors in intact planarians, and following amputation we observed an enrichment of coe + and sim + progenitors near the wound site. RNAi knockdown of coe, hesl-3 or sim led to defects in CNS regeneration, including failure of the cephalic ganglia to properly pattern and a loss of expression of distinct neuronal subtype markers. Together, these data indicate that coe, hesl-3 and sim label neural progenitor cells, which serve to generate new neurons in uninjured or regenerating animals. Our study demonstrates that this model will be useful to investigate how stem cells interpret and respond to genetic and environmental cues in the CNS and to examine the role of bHLH transcription factors in adult tissue regeneration.

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Section: Analysis Of Bhlh Gene Function In Cns Regenerationsupporting

confidence: 76%

Genome-wide analysis of the bHLH gene family in planarians identifies factors required for adult neurogenesis and neuronal regeneration

et al. 2013

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“…quaternary and tertiary), which consist of fewer cells, to the most principal branches, which contain a larger number of gastrodermal cells. Notably, this phenotype differs from those described after silencing other genes required for intestinal integrity (Forsthoefel et al, 2012). The impairment of intestinal adhesion, polarity and phagocyte maturation completely compromises gut regeneration and homeostasis, eventually leading to the death of the animal (Forsthoefel et al, 2012).…”

Section: Egfr-1 Silencing Increases the Number Of Gut Progenitor Cellsmentioning

confidence: 64%

The EGFR signaling pathway controls gut progenitor differentiation during planarian regeneration and homeostasis

2016

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The planarian Schmidtea mediterranea maintains and regenerates all its adult tissues through the proliferation and differentiation of a single population of pluripotent adult stem cells (ASCs) called neoblasts. Despite recent advances, the mechanisms regulating ASC differentiation into mature cell types are poorly understood. Here, we show that silencing of the planarian EGF receptor egfr-1 by RNA interference (RNAi) impairs gut progenitor differentiation into mature cells, compromising gut regeneration and maintenance. We identify a new putative EGF ligand, nrg-1, the silencing of which phenocopies the defects observed in egfr-1(RNAi) animals. These findings indicate that egfr-1 and nrg-1 promote gut progenitor differentiation, and are thus essential for normal cell turnover and regeneration in the planarian gut. Our study demonstrates that the EGFR signaling pathway is an important regulator of ASC differentiation in planarians.

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“…Neoblasts are a heterogeneous population that includes both pluripotent cells and distinct subpopulations specified for production of multiple differentiated tissues (Adler et al, 2014;Cowles et al, 2013;Currie and Pearson, 2013;Forsthoefel et al, 2012;Lapan and Reddien, 2012;Marz et al, 2013;Scimone et al, 2011Scimone et al, , 2014avan Wolfswinkel et al, 2014;Vásquez-Doorman and Petersen, 2014;Vogg et al, 2014;Wenemoser et al, 2012). We hypothesized that notum and wnt11-6 might regulate brain cell production by controlling numbers of brain cell progenitors marked by expression of lineage-specific transcription factors.…”

Section: Planarians Robustly Restore Brain:body Proportionality Throumentioning

confidence: 99%

“…Growth from feeding or epimorphic regeneration depends on parenchymal cells termed neoblasts that are the only proliferating cells in adult planarians (Baguñà, 1976;Newmark and Sánchez Alvarado, 2000;Reddien et al, 2005b). Neoblasts are a heterogeneous population containing both adult pluripotent stem cells (Wagner et al, 2011) and more lineage-restricted dividing cells (Adler et al, 2014;Cowles et al, 2013;Currie and Pearson, 2013;Forsthoefel et al, 2012;Lapan and Reddien, 2012;Marz et al, 2013;Scimone et al, 2014aScimone et al, ,b, 2011van Wolfswinkel et al, 2014;Vásquez-Doorman and Petersen, 2014;Vogg et al, 2014;Wenemoser et al, 2012). Tissue removal results in proliferative activation of neoblasts thought to be necessary for production of missing tissue types within the regeneration blastema.…”

Section: Introductionmentioning

confidence: 99%

Wnt/Notum spatial feedback inhibition controls neoblast differentiation to regulate reversible growth of the planarian brain

2015

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Mechanisms determining final organ size are poorly understood. Animals undergoing regeneration or ongoing adult growth are likely to require sustained and robust mechanisms to achieve and maintain appropriate sizes. Planarians, well known for their ability to undergo whole-body regeneration using pluripotent adult stem cells of the neoblast population, can reversibly scale body size over an order of magnitude by controlling cell number. Using quantitative analysis, we showed that after injury planarians perfectly restored brain:body proportion by increasing brain cell number through epimorphosis or decreasing brain cell number through tissue remodeling (morphallaxis), as appropriate. We identified a pathway controlling a brain size set-point that involves feedback inhibition between wnt11-6/wntA/wnt4a and notum, encoding conserved antagonistic signaling factors expressed at opposite brain poles. wnt11-6/wntA/wnt4a undergoes feedback inhibition through canonical Wnt signaling but is likely to regulate brain size in a non-canonical pathway independently of beta-catenin-1 and APC. Wnt/Notum signaling tunes numbers of differentiated brain cells in regenerative growth and tissue remodeling by influencing the abundance of brain progenitors descended from pluripotent stem cells, as opposed to regulating cell death. These results suggest that the attainment of final organ size might be accomplished by achieving a balance of positional signaling inputs that regulate the rates of tissue production.

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An RNAi Screen Reveals Intestinal Regulators of Branching Morphogenesis, Differentiation, and Stem Cell Proliferation in Planarians

Cited by 120 publications

References 97 publications

Genome-wide analysis of the bHLH gene family in planarians identifies factors required for adult neurogenesis and neuronal regeneration

Genome-wide analysis of the bHLH gene family in planarians identifies factors required for adult neurogenesis and neuronal regeneration

The EGFR signaling pathway controls gut progenitor differentiation during planarian regeneration and homeostasis

Wnt/Notum spatial feedback inhibition controls neoblast differentiation to regulate reversible growth of the planarian brain

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