A mouse model for hereditary thyroid dysgenesis and cleft palate

Felice, Mario De; Ovitt, Catherine E.; Biffali, Elio; Rodríguez-Mallón, Alina; Arra, Claudio; Anastassiadis, Konstantinos; Macchia, Paolo; Mattéi, Marie Geneviève; Mariano, Angela; Schöler, Hans R.; Macchia, Vincenzo; Lauro, Roberto Di

doi:10.1038/1289

Cited by 296 publications

(221 citation statements)

References 19 publications

Supporting

Mentioning

209

Contrasting

Unclassified

Order By: Relevance

“…A homeodomain transcription factor, T/ebp (also called Ttf1, Titf1, or Nkx2.1) (Guazzi et al, 1990;Mizuno et al, 1991), is one of the transcription factors essential for regulating the expression of genes involved in thyroid hormone synthesis as well as thyroid organogenesis (Kimura et al, 1996;De Felice et al, 1998;Mansouri et al, 1998;Damante et al, 2001;Di Lauro and De Felice, 2001;De Felice and Di Lauro, 2004). Mice carrying a null mutation for T/ebp gene die at birth due to profoundly hypoplastic lungs, a defective hypothalamus, and absence of the thyroid and pituitary glands (Kimura et al, 1996).…”

Section: Introductionmentioning

confidence: 99%

Origin of the ultimobranchial body cyst: T/ebp/Nkx2.1 expression is required for development and fusion of the ultimobranchial body to the thyroid

Kusakabe

Hoshi

Kimura

2005

Developmental Dynamics

View full text Add to dashboard Cite

show abstract

Section: Introductionmentioning

confidence: 99%

Origin of the ultimobranchial body cyst: T/ebp/Nkx2.1 expression is required for development and fusion of the ultimobranchial body to the thyroid

Kusakabe

Hoshi

Kimura

2005

Developmental Dynamics

View full text Add to dashboard Cite

show abstract

“…TTF-2 mRNA is expressed in the endoderm lining the foregut, in the developing thyroid, and in the ectoderm that gives rise to the anterior pituitary (Zannini et al, 1997;Parlato et al, 2001). Gene targeting experiments have demonstrated that titf2/foxe1 null mice exhibit cleft palate and either a sublingual or completely absent thyroid gland (De Felice et al, 1998). In humans, mutations of the gene encoding for TTF-2 result in the Bamforth syndrome, characterized by thyroid agenesis, cleft palate, spiky hair, and choanal atresia (Clifton-Bligh et al, 1998).…”

Section: Introductionmentioning

confidence: 99%

Distribution of the titf2/foxe1 gene product is consistent with an important role in the development of foregut endoderm, palate, and hair

Dathan¹,

Parlato

Rosica

et al. 2002

Developmental Dynamics

Self Cite

View full text Add to dashboard Cite

Titf2/foxe1 is a forkhead domain-containing gene expressed in the foregut, in the thyroid, and in the cranial ectoderm of the developing mouse. Titf2 null mice exhibit cleft palate and either a sublingual or completely absent thyroid gland. In humans, mutations of the gene encoding for thyroid transcription factor-2 (TTF-2) result in the Bamforth syndrome, characterized by thyroid agenesis, cleft palate, spiky hair, and choanal atresia. Here, we report a detailed expression pattern of TTF-2 protein during mouse embryogenesis and show its presence in structures where it has not been described yet. At embryonic day (E) 10.5, TTF-2 is expressed in Rathke's pouch, in thyroid, and in the epithelium of the pharyngeal wall and arches, whereas it is absent in the epithelium of the pharyngeal pouches. According to this expression, at E13.5, TTF-2 is present in endoderm derivatives, such as tongue, palate, epiglottis, pharynx, and oesophagus. Later in embryogenesis, we detect TTF-2 in the choanae and whiskers. This pattern of expression helps to define the complex phenotype displayed by human patients. Finally, we show that TTF-2 is a phosphorylated protein. These results help to characterize the domains of TTF-2 expression, from early embryogenesis throughout organogenesis, providing more detail on the potential role of TTF-2 in the development of endoderm and ectoderm derived structures.

show abstract

“…Mice deficient of Nkx2-1, Pax8, Foxe1 or Hhex are well-studied models of athyreosis, i.e. the primordium is correctly specified but eventually regresses leading to a lack of thyroid tissue in late stages of development (Kimura et al, 1996;Mansouri et al, 1998;De Felice et al, 1998;Martinez Barbera et al, 2000). These transcription factors are thus not individually required for thyroid specification or early bud formation.…”

Section: Survival and Growth Of Thyroid Progenitors Depend On A Thyromentioning

confidence: 99%

“…Foxe1 deficient mice are born at an expected ratio but die in the early postnatal period, probably due to the severe cleft palate (De Felice et al, 1998). No orthotopic thyroid is present and hormone analysis reveals severe CH.…”

Section: Foxe1mentioning

confidence: 99%

“…In early thyroid morphogenesis a rudimentary bud is formed but its fate is variable: in 50% of the embryos the thyroid bud retains a position at the base of the prospective tongue, present also in late development (E15.5), whereas in the remainder cases no thyroid is found at all. It has therefore been proposed that Foxe1 specifically regulates the migration of the mouse thyroid primordium after detachment of the bud, besides supporting progenitor cell survival (De Felice et al, 1998), which will be discussed in further detail below (migration section). In contrast, no thyroid phenotype has been identified after knock-down of a recently characterized zebrafish Foxe1 ortholog (see below) (Nakada et al, 2009).…”

Section: Foxe1mentioning

confidence: 99%

See 1 more Smart Citation

Morphogenesis of the thyroid gland

Fagman

Nilsson

2010

Molecular and Cellular Endocrinology

127

View full text Add to dashboard Cite

Congenital hypothyroidism is mainly due to structural defects of the thyroid gland, collectively known as thyroid dysgenesis. The two most prevalent forms of this condition are abnormal localization of differentiated thyroid tissue (thyroid ectopia) and total absence of the gland (athyreosis). The clinical picture of thyroid dysgenesis suggests that impaired specification, proliferation and survival of thyroid precursor cells and loss of concerted movement of these cells in a distinct spatiotemporal pattern are major causes of malformation. In normal development the thyroid primordium is first distinguished as a thickening of the anterior foregut endoderm at the base of the prospective tongue. Subsequently, this group of progenitors detaches from the endoderm, moves caudally and ultimately differentiates into hormone-producing units, the thyroid follicles, at a distant location from the site of specification. In higher vertebrates later stages of thyroid morphogenesis are characterized by shape remodelling into a bilobed organ and the integration of a second type of progenitors derived from the caudal-most pharyngeal pouches that will differentiate into C-cells. The present knowledge of thyroid developmental dynamics has emerged from embryonic studies mainly in chicken, mouse and more recently also in zebrafish. This review will highlight the key morphogenetic steps of thyroid organogenesis and pinpoint which crucial regulatory mechanisms are yet to be uncovered. Considering the coincidence of thyroid dysgenesis and congenital heart malformations the possible interactions between thyroid and cardiovascular development will also be discussed.

show abstract

A mouse model for hereditary thyroid dysgenesis and cleft palate

Cited by 296 publications

References 19 publications

Origin of the ultimobranchial body cyst: T/ebp/Nkx2.1 expression is required for development and fusion of the ultimobranchial body to the thyroid

Origin of the ultimobranchial body cyst: T/ebp/Nkx2.1 expression is required for development and fusion of the ultimobranchial body to the thyroid

Distribution of the titf2/foxe1 gene product is consistent with an important role in the development of foregut endoderm, palate, and hair

Morphogenesis of the thyroid gland

Contact Info

Product

Resources

About