Craniofacial Shape Variation in <i>Twist1<sup>+/−</sup></i> Mutant Mice

Parsons, Trish E.; Weinberg, Seth M.; Khaksarfard, Kameron; Howie, R. Nicole; Elsalanty, Mohammed; Yu, Jack C.; Cray, James J.

doi:10.1002/ar.22899

Cited by 31 publications

(49 citation statements)

References 46 publications

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“…TWIST1 mutations were found in six out of 43 Korean patients (14%) with uni/bicoronal CS, including a single nonsyndromic patient (2.3%) [Ko et al, 2012]. As a further confirmation of the somewhat specific role of TWIST1 in coronal suture patterning, Twist+/− mutant mice exhibit a brachycephalic skull consistent with the involvement of the coronal suture in craniofacial dysmorphism [Parsons et al, 2014]. Based on these facts TWIST1 mutational analysis should be considered for patients with coronal CS even in the absence of clear syndromic traits.…”

Section: Genetic Etiopathogenesis Of Craniosynostosismentioning

confidence: 93%

Genetic advances in craniosynostosis

Lattanzi

Barba

Pietro

et al. 2017

American J of Med Genetics Pt A

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Craniosynostosis, the premature ossification of one or more skull sutures, is a clinically and genetically heterogeneous congenital anomaly affecting approximately 1 in 2,500 live births. In most cases, it occurs as an isolated congenital anomaly, i.e. nonsyndromic craniosynostosis (NCS), the genetic and environmental causes of which remain largely unknown. Recent data suggest that at least some of the midline NCS cases may be explained by two loci inheritance. In approximately 25–30% of patients craniosynostosis presents as a feature of a genetic syndrome due to chromosomal defects or mutations in genes within interconnected signaling pathways. The aim of this review is to provide a detailed and comprehensive update on the genetic and environmental factors associated with NCS, integrating the scientific findings achieved during the last decade. Focus on the neurodevelopmental, imaging and treatment aspects of NCS is also provided.

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Section: Genetic Etiopathogenesis Of Craniosynostosismentioning

confidence: 93%

Genetic advances in craniosynostosis

Lattanzi

Barba

Pietro

et al. 2017

American J of Med Genetics Pt A

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“…Skulls were stabilized using a custom cradle, and reconstructed with NRecon v1.6.4.8 (BrukermicroCT, Kontich, Belgium) as previously described [38]. Threshold settings were set to capture bone volume within the skull.…”

Section: Methodsmentioning

confidence: 99%

Thyroxine Exposure Effects on the Cranial Base

et al. 2017

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Thyroid hormone is important for skull bone growth, which primarily occurs at the cranial sutures and synchondroses. Thyroid hormones regulate metabolism and act in all stages of cartilage and bone development and maintenance by interacting with growth hormone and regulating insulin-like growth factor. Aberrant thyroid hormone levels and exposure during development are exogenous factors that may exacerbate susceptibility to craniofacial abnormalities potentially through changes in growth at the synchondroses of the cranial base. To elucidate the direct effect of in utero therapeutic thyroxine exposure on the synchondroses in developing mice, we provided scaled doses of the thyroid replacement drug, levothyroxine in drinking water to pregnant C57BL6 wild-type dams. The skulls of resulting pups were subjected to microcomputed tomography analysis revealing less bone volume relative to tissue volume in the synchondroses of mouse pups exposed in utero to levothyroxine. Histological assessment of the cranial base area indicated more active synchondroses as measured by metabolic factors including Igf1. The cranial base of the pups exposed to high levels of levothyroxine also contained more collagen fiber matrix and an increase in markers of bone formation. Such changes due to exposure to exogenous thyroid hormone may drive overall morphological changes. Thus, excess thyroid hormone exposure to the fetus during pregnancy may lead to altered craniofacial growth and increased risk of anomalies in offspring.

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“…Scans were obtained on 181 animals (Male = 42.8%; Female = 43.3%; Undetermined = 13.9%). Mouse skulls were reconstructed with NRecon v1.6.4.8 (BrukermicroCT, Kontich, Belgium) as previously described and imported into Amira v5.0 where it was exposed to a Gaussian Smoothing image filter (r50.3 in X, Y, and Z dimensions; isometric kernel size53) to reduce extraneous noise in the images [47]. Threshold settings were then set to only visualize bone volume within the skull.…”

Section: Methodsmentioning

confidence: 99%

Effects of In Utero Thyroxine Exposure on Murine Cranial Suture Growth

Howie¹,

Durham²,

Black³

et al. 2016

PLoS ONE

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Large scale surveillance studies, case studies, as well as cohort studies have identified the influence of thyroid hormones on calvarial growth and development. Surveillance data suggests maternal thyroid disorders (hyperthyroidism, hypothyroidism with pharmacological replacement, and Maternal Graves Disease) are linked to as much as a 2.5 fold increased risk for craniosynostosis. Craniosynostosis is the premature fusion of one or more calvarial growth sites (sutures) prior to the completion of brain expansion. Thyroid hormones maintain proper bone mineral densities by interacting with growth hormone and aiding in the regulation of insulin like growth factors (IGFs). Disruption of this hormonal control of bone physiology may lead to altered bone dynamics thereby increasing the risk for craniosynostosis. In order to elucidate the effect of exogenous thyroxine exposure on cranial suture growth and morphology, wild type C57BL6 mouse litters were exposed to thyroxine in utero (control = no treatment; low ~167 ng per day; high ~667 ng per day). Thyroxine exposed mice demonstrated craniofacial dysmorphology (brachycranic). High dose exposed mice showed diminished area of the coronal and widening of the sagittal sutures indicative of premature fusion and compensatory growth. Presence of thyroid receptors was confirmed for the murine cranial suture and markers of proliferation and osteogenesis were increased in sutures from exposed mice. Increased Htra1 and Igf1 gene expression were found in sutures from high dose exposed individuals. Pathways related to the HTRA1/IGF axis, specifically Akt and Wnt, demonstrated evidence of increased activity. Overall our data suggest that maternal exogenous thyroxine exposure can drive calvarial growth alterations and altered suture morphology.

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Craniofacial Shape Variation in Twist1^+/− Mutant Mice

Cited by 31 publications

References 46 publications

Genetic advances in craniosynostosis

Genetic advances in craniosynostosis

Thyroxine Exposure Effects on the Cranial Base

Effects of In Utero Thyroxine Exposure on Murine Cranial Suture Growth

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Craniofacial Shape Variation in Twist1+/− Mutant Mice

Cited by 31 publications

References 46 publications

Genetic advances in craniosynostosis

Genetic advances in craniosynostosis

Thyroxine Exposure Effects on the Cranial Base

Effects of In Utero Thyroxine Exposure on Murine Cranial Suture Growth

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Product

Resources

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Craniofacial Shape Variation in Twist1^+/− Mutant Mice