Human and mouse<i>TPIT</i>gene mutations cause early onset pituitary ACTH deficiency

Pulichino, Anne-Marie; Vallette-Kasic, Sophie; Couture, Catherine; Gauthier, Yves; Brue, Thierry; Dávid, M; Malpuech, G; Deal, Cheri; Vliet, Guy Van; Vroede, Monique De; Riepe, Felix G.; Partsch, Carl-Joachim; Sippell, Wolfgang G.; Berberoğlu, Merih; Atasay, Begüm; Drouin, Jacques

doi:10.1101/gad.1065603

Cited by 196 publications

(137 citation statements)

References 36 publications

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“…Ainsi, par l'analyse de la séquence codante du gène TPIT dans une série de 17 patients présentant un déficit corticotrope isolé congénital, nous avons montré que les mutations de TPIT sont associées à un déficit congénital isolé en ACTH dans 8 cas sur 11 pour lesquels ce déficit est précoce (néona-tal). En revanche, lorsque ce déficit apparaît plus tardivement dans l'enfance, nous n'avons pas mis en évidence de mutations de TPIT (6/6 cas) [7]. Les patients sans mutation de TPIT n'avaient pas d'antécédent familial de déficit corticotrope (qu'il soit juvénile ou néonatal).…”

Section: Déficit Corticotrope Isolé Congénitalunclassified

“…Afin de déterminer la cause du déficit produit par les trois mutations faux-sens (T58A, I171T, S128F), nous avons inséré ces mutations dans des vecteurs d'expression et avons testé leur activité transcriptionnelle en transfections transitoires, ainsi que leur capacité de liaison à l'ADN. Les protéines mutantes ont une perte de leur activité transcriptionnelle, avec une absence de liaison à l'ADN [7]. Ces trois mutations affectent la boîte T de la protéine, notamment la thréonine en position 58 impliquée dans la liaison à l'ADN [15].…”

Section: Déficit Corticotrope Isolé Congénitalunclassified

“…Chez la souris, son expression est restreinte aux deux lignées hypophysaires exprimant la POMC, les cellules corticotropes et les cellules mélanotropes [6]. Nous avons identifié plusieurs mutations du gène TPIT chez des patients atteints de déficit corticotrope isolé congénital, permettant de mieux définir cette entité cli- nique et d'y apporter une explication moléculaire [7]. Postulant que la souris serait un bon modèle du déficit corticotrope isolé congénital, nous avons produit une souris dont le gène Tpit a été invalidé.…”

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Mutations du facteur de transcription Tpitet différenciation hypophysaire

et al. 2004

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Section: Déficit Corticotrope Isolé Congénitalunclassified

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Mutations du facteur de transcription Tpitet différenciation hypophysaire

et al. 2004

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“…11,12 In addition, Tbx1 mutations result in DiGeorge syndrome, Tbx19 mutations are found in patients with adrenocorticotrophin (ACTH) deficiency in the pituitary, and Tbx22 mutations are associated with cleft lip and palate. [13][14][15] Taken together, it is clear that disrupting T-box factor activity has severe consequences for human health.…”

Section: T-box Transcription Factor Familymentioning

confidence: 99%

An essential interaction between T-box proteins and histone-modifying enzymes

Miller

Weinmann

2009

Epigenetics

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Cellular differentiation requires precisely coordinated events to induce developmentally appropriate gene expression profiles. Lineage-defining transcription factors are responsible for establishing cell-type specific gene expression patterns during development. Recently, we reported a novel mechanism by which the T-box transcription factor T-bet interacts with JMJD3, an H3K27-demethylase, and Set7/9, an H3K4-methyltransferase (Genes Dev 2008; 22:2980-93). Importantly, separable contact points in the T-box DNA binding domain mediate these interactions. Due to the highly conserved nature of the contact residues, these represent common interactions for the T-box family. Therefore, studies examining the molecular mechanisms that account for the ability of T-bet to regulate Ifng and Cxcr3, prototypic CD4 + Th1 genes, have provided novel insight into essential regulatory events that occur at diverse developmental transitions. In this article, we discuss the implications for these findings as well as explore the role epigenetic mechanisms may play in the development of human genetic diseases that are caused by T-box mutations, including congenital heart defects, cleft palate, pituitary deficiencies and Ulnar-mammary syndrome.

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“…Mutations in Pit1 or Prop1 result in a failure of Pit1 lineages differentiation, leading to a postnatal dwarf phenotype. Terminal differentiation of corticotropes and melanotropes is dependent on the T-box transcription factor, Tbx19 [8]. Here we highlight the recent progress in our understanding of the mechanisms underlying pituitary organogenesis, filling the gap between signaling pathways and transcription factors.…”

Section: Introductionmentioning

confidence: 99%

Signaling and epigenetic regulation of pituitary development

Zhu

Wang

et al. 2007

Current Opinion in Cell Biology

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The developing pituitary gland provides an instructive model system for elucidating the molecular mechanisms by which distinct cell types arise from a common progenitor lineage accompanied by changes in the chromatin status in response to multiple extrinsic and intrinsic signals. Recent studies have shed light on the integration between signaling molecules and activation of transcription factors that are essential for cell fate commitment and terminal differentiation. Investigation of the in vivo function of the histone modifying enzyme LSD1 has revealed a new layer of regulatory mechanism in pituitary organogenesis. Epigenetic studies of the transcriptional events in terminal differentiation process have provided insights into the functions of non-coding RNA and developmentally regulated chromatin organization.

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Human and mouseTPITgene mutations cause early onset pituitary ACTH deficiency

Cited by 196 publications

References 36 publications

Mutations du facteur de transcription Tpitet différenciation hypophysaire

Mutations du facteur de transcription Tpitet différenciation hypophysaire

An essential interaction between T-box proteins and histone-modifying enzymes

Signaling and epigenetic regulation of pituitary development

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