FoxO6 regulates Hippo signaling and growth of the craniofacial complex

Sun, Zhao; Fontoura, Clarissa Souza Gomes da; Moreno, Myriam; Holton, Nathan E.; Sweat, Mason; Sweat, Yan Yan; Lee, Myoung Keun; Arbon, Jed; Bidlack, Felicitas B.; Thedens, Daniel R.; Nopoulos, Peg; Cao, Huojun; Eliason, Steven; Weinberg, Seth M.; Martin, James F.; Moreno‐Uribe, Lina; Amendt, Brad A.

doi:10.1371/journal.pgen.1007675

Cited by 31 publications

(26 citation statements)

References 166 publications

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“…The four FoxO protein members share obvious sequence homology and possess four clearly different functional motifs, which include a forkhead domain, nuclear localization, nuclear export, and transactivation domains ( Figure 1) [12,13]. All the four FoxO members are ubiquitously expressed [14], including FoxO6 that was previously reported to exist basically in the brain but has been more recently discovered in other organs as well [4,15]. In particular, FoxO1, FoxO4, and FoxO6 are more detected in the adipose, musculoskeletal, and nervous tissues, respectively, while FoxO3 is more expressed in the stomach, spleen, kidney, intestine, and cardiac tissues [13].…”

Section: The Foxo Familymentioning

confidence: 99%

The Roles of FoxO Transcription Factors in Regulation of Bone Cells Function

Chen

et al. 2020

IJMS

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Forkhead box class O family member proteins (FoxOs) are evolutionarily conserved transcription factors for their highly conserved DNA-binding domain. In mammalian species, all the four FoxO members, FoxO1, FoxO3, FoxO4, and FoxO6, are expressed in different organs. In bone, the first three members are extensively expressed and more studied. Bone development, remodeling, and homeostasis are all regulated by multiple cell lineages, including osteoprogenitor cells, chondrocytes, osteoblasts, osteocytes, osteoclast progenitors, osteoclasts, and the intercellular signaling among these bone cells. The disordered FoxOs function in these bone cells contribute to osteoarthritis, osteoporosis, or other bone diseases. Here, we review the current literature of FoxOs for their roles in bone cells, focusing on helping researchers to develop new therapeutic approaches and prevent or treat the related bone diseases.

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Section: The Foxo Familymentioning

confidence: 99%

The Roles of FoxO Transcription Factors in Regulation of Bone Cells Function

Chen

et al. 2020

IJMS

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“…Even though both FOXO6 and POU3F1 are transcription factors, they play distinguishable roles in the regulation of gene expression. Foxo6 is expressed at late stages of face development [71]. Foxo6 -/mice underwent expansion of the face, frontal cortex, olfactory component and skull [71].…”

Section: Several Candidate Icr Map To the Vicinity Of Genes Encoding mentioning

confidence: 99%

“…Foxo6 is expressed at late stages of face development [71]. Foxo6 -/mice underwent expansion of the face, frontal cortex, olfactory component and skull [71]. Pou3f1 plays a role in spermatogenesis [72].…”

Section: Several Candidate Icr Map To the Vicinity Of Genes Encoding mentioning

confidence: 99%

“…Cited2 impacts left-right patterning of the body' s axis [33]. Functions of FOXO6 include regulation of Hippo signaling and the growth of the craniofacial complex [71]. In the context of organogenesis, we obtained Maml3.…”

Section: Several Of the Candidate Icrs Map To Genes With Functions Ramentioning

confidence: 99%

“…This gene encodes a transcription factor. Its functions include regulation of Hippo signaling and growth of the craniofacial complex[71].______________________________________________________________________________________ Fig. S23.…”

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Simultaneous discovery of candidate imprinted genes and Imprinting Control Regions in the mouse genome

Bina

Wyss

2019

Preprint

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In mammals, parent-of-origin-specific gene expression is regulated by specific genomic DNA segments known as Imprinting Control Regions (ICRs) and germline Differentially Methylated Regions (gDMRs). In the mouse genome, the known ICRs/gDMRs often include clusters of a set of composite-DNA-elements known as ZFBS-morph overlaps. These elements consist of the ZFP57 binding site (ZFBS) overlapping a subset of the MLL1 morphemes. To improve detection of such clusters, we created density-plots. In genome-wide analyses, peaks in these plots pinpointed ~90% of the known ICRs/gDMRs and located candidate ICRs within relatively long genomic DNA sections. In several cases, the candidate ICRs mapped to chromatin boundaries, to a subset of gene-transcripts, or to both. By viewing the plots at the UCSC genome browser, we could examine the candidate ICRs in the context of the genes in their vicinity. This strategy uncovered several potential imprinted genes with a broad range of physiologically important functions. Examples include: folliculogenesis; lineage commitment of murine embryonic stem cells; the development of the junctional zone of the placenta; left-right patterning of the body axis; the development of the neocortex, hippocampus, and cerebellum; postnatal vision; self-renewal of mouse spermatogonial stem cells; and histone-to-protamine replacement during spermatogenesis. Predicted imprinted genes: Arid1b,

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ThemiR-200family is required for ectodermal organ development through the regulation of the epithelial stem cell niche

Sweat

et al. 2021

Stem Cells

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The murine lower incisor ectodermal organ contains a single epithelial stem cell (SC) niche that provides epithelial progenitor cells to the continuously growing rodent incisor. The dental stem cell niche gives rise to several cell types and we demonstrate that the miR-200 family regulates these cell fates. The miR-200 family is highly enriched in the differentiated dental epithelium and absent in the stem cell niche. In this study, we inhibited the miR-200 family in developing murine embryos using new technology, resulting in an expanded epithelial stem cell niche and lack of cell differentiation. Inhibition of individual miRs within the miR-200 cluster resulted in differential developmental and cell morphology defects. miR-200 inhibition increased the expression of dental epithelial stem cell markers, expanded the stem cell niche and decreased progenitor cell differentiation. RNA-seq. identified miR-200 regulatory pathways involved in cell differentiation and compartmentalization of the stem cell niche. The miR-200 family regulates signaling pathways required for cell differentiation and cell cycle progression. The inhibition of miR-200 decreased the size of the lower incisor due to increased autophagy and cell death. New miR-200 targets demonstrate gene networks and pathways controlling cell differentiation and maintenance of the stem cell niche. This is the first report demonstrating how the miR-200 family is required for in vivo progenitor cell proliferation and differentiation.

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FoxO6 regulates Hippo signaling and growth of the craniofacial complex

Cited by 31 publications

References 166 publications

The Roles of FoxO Transcription Factors in Regulation of Bone Cells Function

The Roles of FoxO Transcription Factors in Regulation of Bone Cells Function

Simultaneous discovery of candidate imprinted genes and Imprinting Control Regions in the mouse genome

ThemiR-200family is required for ectodermal organ development through the regulation of the epithelial stem cell niche

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