A regulatory feedback loop involving p63 and IRF6 links the pathogenesis of 2 genetically different human ectodermal dysplasias

Moretti, Francesca; Marinari, Barbara; Iacono, Nadia Lo; Botti, Elisabetta; Giunta, Alessandro; Spallone, Giulia; Garaffo, Giulia; Vernersson-Lindahl, Emma; Merlo, Giorgio R.; Mills, Alea A.; Ballarò, Costanza; Alemà, Stefano; Chimenti, Sergio; Guerrini, Luisa; Costanzo, Antonio

doi:10.1172/jci40267

Cited by 127 publications

(209 citation statements)

References 30 publications

(44 reference statements)

Supporting

Mentioning

183

Contrasting

Order By: Relevance

“…38 This increase in IRF6 may then lead to p63 degradation in keratinocytes, thereby restricting the proliferative potential and promoting keratinocyte differentiation. 39 Our data do not exclude that under certain conditions an interplay between IRF6 and p63 directly enhances RIPK4 promoter activity.…”

Section: G H and I)contrasting

confidence: 66%

A novel RIPK4–IRF6 connection is required to prevent epithelial fusions characteristic for popliteal pterygium syndromes

et al. 2014

View full text Add to dashboard Cite

Receptor-interacting protein kinase 4 (RIPK4)-deficient mice have epidermal defects and fusion of all external orifices. These are similar to Bartsocas-Papas syndrome and popliteal pterygium syndrome (PPS) in humans, for which causative mutations have been documented in the RIPK4 and IRF6 (interferon regulatory factor 6) gene, respectively. Although genetically distinct, these syndromes share the anomalies of marked pterygia, syndactyly, clefting and hypoplastic genitalia. Despite the strong resemblance of these two syndromes, no molecular connection between the transcription factor IRF6 and the kinase RIPK4 was known and the mechanism underlying the phenotype was unclear. Here we describe that RIPK4 deficiency in mice causes epithelial fusions associated with abnormal periderm development and aberrant ectopic localization of E-cadherin on the apical membrane of the outer peridermal cell layers. In Xenopus, RIPK4 depletion causes the absence of ectodermal epiboly and concomitant gastrulation defects that phenocopy ectopic expression of dominant-negative IRF6. We found that IRF6 controls RIPK4 expression and that wild-type, but not kinase-dead, RIPK4 can complement the gastrulation defect in Xenopus caused by IRF6 malfunctioning. In contrast to the mouse, we observed only minor effects on cadherin membrane expression in Xenopus RIPK4 morphants. However, gastrulation defects were associated with a virtual absence of cortical actin in the ectodermal cells that face the blastocoel cavity and this was phenocopied in embryos expressing dominant-negative IRF6. A role for RIPK4 in actin cytoskeleton organization was also revealed in mouse epidermis and in human epithelial HaCaT cells. In conclusion, we showed that in mice RIPK4 is implicated in cortical actin organization and in E-cadherin localization or function, which can explain the characteristic epithelial fusions observed in PPSs. In addition, we provide a novel molecular link between IRF6 and RIPK4 that unifies the different PPSs to a common molecular pathway.

show abstract

Section: G H and I)contrasting

confidence: 66%

A novel RIPK4–IRF6 connection is required to prevent epithelial fusions characteristic for popliteal pterygium syndromes

et al. 2014

View full text Add to dashboard Cite

show abstract

“…N1ICD binds to the IRF6 gene in keratinocytes and activates its expression (33). In turn, IRF6 promotes proteasomal degradation of p63 (30). An analogous mechanism could regulate p63 in vCTBs, because IRF6 rapidly increased after N1ICD expression.…”

Section: Discussionmentioning

confidence: 99%

“…S8). In addition, N1ICD increased expression of IFN regulatory factor 6 (IRF6), a negative regulator of p63 (30) (Fig. 5 D and F and SI Appendix, Fig.…”

Section: Ectopic Notch1 Induces An Extravillous Trophoblast Progenitomentioning

confidence: 99%

Notch1 controls development of the extravillous trophoblast lineage in the human placenta

Haider

Meinhardt

Saleh

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

115

144

View full text Add to dashboard Cite

Development of the human placenta and its different epithelial trophoblasts is crucial for a successful pregnancy. Besides fusing into a multinuclear syncytium, the exchange surface between mother and fetus, progenitors develop into extravillous trophoblasts invading the maternal uterus and its spiral arteries. Migration into these vessels promotes remodelling and, as a consequence, adaption of blood flow to the fetal–placental unit. Defects in remodelling and trophoblast differentiation are associated with severe gestational diseases, such as preeclampsia. However, mechanisms controlling human trophoblast development are largely unknown. Herein, we show that Notch1 is one such critical regulator, programming primary trophoblasts into progenitors of the invasive differentiation pathway. At the 12th wk of gestation, Notch1 is exclusively detected in precursors of the extravillous trophoblast lineage, forming cell columns anchored to the uterine stroma. At the 6th wk, Notch1 is additionally expressed in clusters of villous trophoblasts underlying the syncytium, suggesting that the receptor initiates the invasive differentiation program in distal regions of the developing placental epithelium. Manipulation of Notch1 in primary trophoblast models demonstrated that the receptor promotes proliferation and survival of extravillous trophoblast progenitors. Notch1 intracellular domain induced genes associated with stemness of cell columns, myc and VE-cadherin, in Notch1−fusogenic precursors, and bound to themycpromoter and enhancer region at RBPJκ cognate sequences. In contrast, Notch1 repressed syncytialization and expression of TEAD4 and p63, two regulators controlling self-renewal of villous cytotrophoblasts. Our results revealed Notch1 as a key factor promoting development of progenitors of the extravillous trophoblast lineage in the human placenta.

show abstract

“…We found that p21 expression was restored in E14. Previous studies have demonstrated that IRF6 induces degradation of the p63 isoform ∆Np63 and that this is linked with the pathogenesis of VWS and PPS (Moretti et al, 2010;Thomason et al, 2010). In addition, ∆Np63 represses transcription of p21 in vitro and in vivo (Laurikkala et al, 2006;Welsh and O'Brien, 2009;Westfall et al, 2003).…”

Section: Irf6 Regulates Mee Disappearance Via P21 Expressionmentioning

confidence: 95%

“…Among the genes that have been associated with NSCL/P, IRF6 has been implicated in the largest percentage of cases (Koillinen et al, 2005;Srichomthong et al, 2005). Mutation of IRF6 can lead to the autosomal-dominant conditions VWS and PPS, which are characterized by oral clefting and lower lip pits (Kondo et al, 2002;Moretti et al, 2010). VWS and PPS are allelic variants of the same condition caused by different mutations of the same gene.…”

Section: Introductionmentioning

confidence: 99%

Smad4-Irf6 genetic interaction and TGFβ-mediated IRF6 signaling cascade are crucial for palatal fusion in mice

et al. 2013

View full text Add to dashboard Cite

SUMMARYCleft palate is one of the most common human birth defects and is associated with multiple genetic and environmental risk factors. Although mutations in the genes encoding transforming growth factor beta (TGFβ) signaling molecules and interferon regulatory factor 6 (Irf6) have been identified as genetic risk factors for cleft palate, little is known about the relationship between TGFβ signaling and IRF6 activity during palate formation. Here, we show that TGFβ signaling regulates expression of Irf6 and the fate of the medial edge epithelium (MEE) during palatal fusion in mice. Haploinsufficiency of Irf6 in mice with basal epithelial-specific deletion of the TGFβ signaling mediator Smad4 (Smad4

show abstract

A regulatory feedback loop involving p63 and IRF6 links the pathogenesis of 2 genetically different human ectodermal dysplasias

Cited by 127 publications

References 30 publications

A novel RIPK4–IRF6 connection is required to prevent epithelial fusions characteristic for popliteal pterygium syndromes

A novel RIPK4–IRF6 connection is required to prevent epithelial fusions characteristic for popliteal pterygium syndromes

Notch1 controls development of the extravillous trophoblast lineage in the human placenta

Smad4-Irf6 genetic interaction and TGFβ-mediated IRF6 signaling cascade are crucial for palatal fusion in mice

Contact Info

Product

Resources

About