Craniofacial features resembling frontonasal dysplasia with a tubulonodular interhemispheric lipoma in the adult 3H1 <i>tuft</i> mouse

Fong, Keith S. K.; Cooper, Tiffiny Baring; Drumhiller, Wallace C.; Somponpun, Suwit J.; Yang, Shiming; Ernst, Thomas; Chang, Linda; Lozanoff, Scott

doi:10.1002/bdra.22878

Cited by 3 publications

(27 citation statements)

References 52 publications

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“…The etiology of FND is thought to be a developmental field defect affecting features along the frontonasal midline during morphogenesis of the facial bones and tissues (DeMeyer, ; Sedano, ; Cohen et al, ; Wu et al, ; Guion‐Almeida and Richieri‐Costa, ). Cephaloceles, cranium bifidum, ocular hypertelorism, a bifid nose, and midfacial cleft are features of FND that were observed in the tuft mouse (Fong et al, ). Consistent with the clinical manifestations of FND, each of these traits in tuft mice did not necessarily occur together in the same animal, nor did they occur to the same degree.…”

Section: Discussionmentioning

confidence: 99%

“…We have identified a candidate region on mouse Chromosome 10 that contain several loci associated with cellular adhesion (Fong et al, ). Most notably is Alx1, which along with Alx3 and Alx4, were found mutated in humans with FND‐like defects (Kayserili et al, ; Twigg et al, ; Uz et al, ).…”

Section: Discussionmentioning

confidence: 99%

“…All procedures were carried out in accordance with Institutional Animal Care & Use Committee specifications and performed following protocols approved by the University of Hawai'i Laboratory of Animal Services. Mice strains were housed under standard conditions and bred as previously described (Fong et al, ). Timed matings were determined by noting the presence of a vaginal plug as day 0.5 for staging embryo collections and estimating date of births.…”

Section: Methodsmentioning

confidence: 99%

“…Whole‐mount staining of newborn skulls with Alcian blue and Alizarin red were previously described (Fong et al, ). Each mouse cranium was observed with a Leitz dissection microscope and digitally documented (Olympus Imaging America Inc., Center Valley, PA).…”

Section: Methodsmentioning

confidence: 99%

“…We recently described the tuft mouse with heritable craniofacial malformations resembling frontonasal dysplasia (FND) featuring an interhemispheric lipoma. Affected adults exhibited one or more craniofacial malformations that included ocular hypertelorism, frontonasal cleft (bifid nose), shortened and sloping nasal ridge, and a lipomatous extracranial mass emanating from the anterior part of the skull (Fong et al, ). Histological and imaging analysis indicated that the lipomatous mass was an extension of the meninges protruding through an opening along the sagittal suture, usually between the paired frontal bones of the mouse.…”

Section: Introductionmentioning

confidence: 99%

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Midline craniofacial malformations with a lipomatous cephalocele are associated with insufficient closure of the neural tube in the tuft mouse

Fong

Adachi

Chang

et al. 2014

Birth Defects Research

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Genetic variations affecting neural tube closure along the head result in malformations to the face and brain, posing a significant impact on health care costs and the quality of life. We have established a mouse line from a mutation that arose spontaneously in our wildtype colony that we called tuft. Tuft mice have heritable midline craniofacial defects featuring an anterior lipomatous cephalocele. Whole mount skeletal stains indicated that affected newborns had a broader interfrontal suture where the cephalocele emerged between the frontal bones. Mice with a cephalocele positioned near the rostrum also presented craniofacial malformations such as ocular hypertelorism and midfacial cleft of the nose. Gross and histological examination revealed that the lipomatous cephalocele originated as a fluid filled cyst no earlier than E14.5 while embryos with a midfacial cleft was evident during craniofacial development at E11.5. Histological sections of embryos with a midfacial cleft revealed the cephalic neuroectoderm remained proximal or fused to the frontonasal ectoderm about the closure site of the anterior neuropore, indicating a defect to neural tube closure. We found the neural folds along the rostrum of E9-10.5 embryos curled inward and failed to close as well as embryos with exencephaly and anencephaly at later stages. Whole mount in situ hybridization of anterior markers Fgf8 and Shh indicated closure of the rostral site was compromised in severe cases. We present a model demonstrating how anterior cranial cephaloceles are generated following a defect to neural tube closure and relevance to subsequent craniofacial morphogenesis in the tuft mouse.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Midline craniofacial malformations with a lipomatous cephalocele are associated with insufficient closure of the neural tube in the tuft mouse

Fong

Adachi

Chang

et al. 2014

Birth Defects Research

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A mutation in the tuft mouse disrupts TET1 activity and alters the expression of genes that are crucial for neural tube closure

Fong

Hufnagel

Khadka

et al. 2016

Disease Models &Amp; Mechanisms

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Genetic variations affecting neural tube closure along the head result in malformations of the face and brain. Neural tube defects (NTDs) are among the most common birth defects in humans. We previously reported a mouse mutant called tuft that arose spontaneously in our wild-type 3H1 colony. Adult tuft mice present midline craniofacial malformations with or without an anterior cephalocele. In addition, affected embryos presented neural tube closure defects resulting in insufficient closure of the anterior neuropore or exencephaly. Here, through whole-genome sequencing, we identified a nonsense mutation in the Tet1 gene, which encodes a methylcytosine dioxygenase (TET1), co-segregating with the tuft phenotype. This mutation resulted in premature termination that disrupts the catalytic domain that is involved in the demethylation of cytosine. We detected a significant loss of TET enzyme activity in the heads of tuft embryos that were homozygous for the mutation and had NTDs. RNA-Seq transcriptome analysis indicated that multiple gene pathways associated with neural tube closure were dysregulated in tuft embryo heads. Among them, the expressions of Cecr2, Epha7 and Grhl2 were significantly reduced in some embryos presenting neural tube closure defects, whereas one or more components of the non-canonical WNT signaling pathway mediating planar cell polarity and convergent extension were affected in others. We further show that the recombinant mutant TET1 protein was capable of entering the nucleus and affected the expression of endogenous Grhl2 in IMCD-3 (inner medullary collecting duct) cells. These results indicate that TET1 is an epigenetic determinant for regulating genes that are crucial to closure of the anterior neural tube and its mutation has implications to craniofacial development, as presented by the tuft mouse.

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The Unicorn Mouse: Cranial Lipoma in a B6.Cg Mouse

Duncan¹,

Helke²

2022

BJVP

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Intracranial lipomas, also called intracranial lipomatous hamartomas, have been reported in some strains of research mice, but are rare in C57BL6 strains. It is presumed based on current publications that this is the first report of an intracranial lipoma in a mouse with this genetic change (B6.Cg-Cnpy2 tm1.2 Zhli Alb-Cre). Grossly, a fur-covered, soft, cylindrical, exophytic mass on the dorsal midline of the cranium was evident. Upon dissection, a soft, white, tubular structure extended through a 1mm defect in the sagittal suture of the skull to the deep surface of the hypodermis. Histologically, the mass consisted of well demarcated proliferation of mature white adipocytes, each containing one large fat droplet. The mass extended from the cerebrum at the level just caudal to the hippocampus in the third ventricle, between the superior colliculus and the caudal portion of the retrosplenial area and through the sagittal suture to the hypodermis and was surrounded by normal brain tissue.

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Craniofacial features resembling frontonasal dysplasia with a tubulonodular interhemispheric lipoma in the adult 3H1 tuft mouse

Cited by 3 publications

References 52 publications

Midline craniofacial malformations with a lipomatous cephalocele are associated with insufficient closure of the neural tube in the tuft mouse

Midline craniofacial malformations with a lipomatous cephalocele are associated with insufficient closure of the neural tube in the tuft mouse

A mutation in the tuft mouse disrupts TET1 activity and alters the expression of genes that are crucial for neural tube closure

The Unicorn Mouse: Cranial Lipoma in a B6.Cg Mouse

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