PAX8,TITF1, andFOXE1Gene Expression Patterns during Human Development: New Insights into Human Thyroid Development and Thyroid Dysgenesis-Associated Malformations

旅客8 甲状腺 肾脏发育 生物 间充质 前脑 发育不良 病理 内科学 医学 内分泌学 解剖 基因 胚胎干细胞 中枢神经系统 上皮 遗传学 转录因子
作者
Sylvia Sura Trueba,Joëlle Augé,Géraldine Mattei,Heather Etchevers,Jélééna Martinovic,Paul Czernichow,Michel Vekemans,Michel Polak,Tania Attié‐Bitach
出处
期刊:The Journal of Clinical Endocrinology and Metabolism [Oxford University Press]
卷期号:90 (1): 455-462 被引量:215
标识
DOI:10.1210/jc.2004-1358
摘要

Thyroid dysgenesis (TD) is responsible for most cases of congenital hypothyroidism, a condition that affects about one in 4000 newborns. Mutations in PAX8, TITF1, or FOXE1 may account for congenital hypothyroidism in patients with either isolated TD or TD with associated malformations involving kidney, lung, forebrain, and palate. Pax8, titf1, and foxe1 are expressed in the mouse thyroid bud as soon as it differentiates on the pharyngeal floor. Because the spatio-temporal expression of these genes is unknown in humans, we decided to study them at different stages of human embryonic and fetal development. PAX8 and TITF1 were first expressed in the median thyroid primordium. Interestingly, PAX8 was also expressed in the thyroglossal duct and the ultimobranchial bodies. Human FOXE1 expression was detected later than in the mouse. PAX8 was also expressed in the developing central nervous system and kidney, including the ureteric bud and the main collecting ducts. TITF1 was expressed in the ventral forebrain and lung. FOXE1 expression was detected in the oropharyngeal epithelium and thymus. In conclusion, the expression patterns described here show some differences from those reported in the mouse. They explain the malformations associated with TD in patients carrying PAX8, TITF1, and FOXE1 gene mutations.
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