par Grasberger, Helmut;Vaxillaire, Martine;Pannain, Silvana;Beck, John C;Mimouni-Bloch, Aviva;Vatin, Vincent;Vassart, Gilbert 
;Froguel, Philippe;Refetoff, Samuel
Référence Human genetics, 118, 3-4, page (348-355)
Publication Publié, 2005-12
;Froguel, Philippe;Refetoff, Samuel Référence Human genetics, 118, 3-4, page (348-355)
Publication Publié, 2005-12
Article révisé par les pairs
| Résumé : | Permanent congenital hypothyroidism is the most prevalent inborn endocrine disorder, and principally due to developmental defects leading to absent, ectopic or hypoplastic thyroid gland. Although commonly regarded as sporadic disease, nonsyndromic thyroid hypoplasia has, in rare cases, been attributed to inherited defects in PAX8 and the TSHR gene. The shared clinical picture caused by these defects is a variable degree of thyrotropin resistance (RTSH [MIM 275200]), accompanied in its severe form by thyroid gland hypoplasia. We recently identified six extended kindreds with autosomal dominant RTSH, only one of which was linked to a mutation in the PAX8 candidate gene. Genome wide scans conducted in two of the remaining five families revealed independently significant linkage to chromosome 15q25.3-26.1, with maximum multipoint LOD scores of 8.51 and 4.31. Linkage to this novel locus was replicated (P<0.01) in each of the three remaining kindreds. Fine mapping of key recombinants in the largest family localized the causative gene within a 3 cM/2.9 Mb interval. Thus, we report the first locus for congenital nongoitrous hypothyroidism identified by a genome wide screening approach. |
