首页> 外文期刊>Human Molecular Genetics >A novel loss-of-function mutation in TTF-2 is associated with congenital hypothyroidism, thyroid agenesis and cleft palate.
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A novel loss-of-function mutation in TTF-2 is associated with congenital hypothyroidism, thyroid agenesis and cleft palate.

机译:TTF-2的新型功能丧失突变与先天性甲状腺功能减退,甲状腺发育不全和c裂有关。

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摘要

Thyroid dysgenesis is the most common cause of congenital hypothyroidism (CH) and its genetic basis is largely unknown. Here, we describe the second homozygous missense mutation in TTF-2 (or FOXE1), a transcription factor that has been implicated in thyroid development. Two male siblings, born to consanguineous parents, presented with CH, athyreosis and cleft palate and were found to be homozygous for a mutation corresponding to a serine to asparagine substitution at codon 57 (S57N) in the forkhead DNA binding domain of TTF-2. Their heterozygous parents were unaffected and this mutation was not found in 31 unrelated cases of athyreosis or normal controls. Consistent with its location, the S57N TTF-2 mutant protein showed impaired DNA binding and partial loss of transcriptional function. Such incomplete loss of TTF-2 function may account for the absence of choanal atresia and bifid epiglottis in our patients, anomalies which were present together with CH and cleft palate in two other individuals with the only other, more deleterious, TTF-2 mutation (A65V) described previously. Our observations support the role of TTF-2 in both thyroid and palate development but suggest phenotypic heterogeneity of this syndromic form of CH.
机译:甲状腺功能不全是先天性甲状腺功能减退症(CH)的最常见原因,其遗传基础尚不明确。在这里,我们描述了TTF-2(或FOXE1)中的第二个纯合错义突变,该转录因子已与甲状腺发育有关。两名近亲父母所生的男性兄弟姐妹患有CH,无胸腺病和c裂,被发现在TTF-2前叉DNA结合域中对应于第57位密码子(S57N)的丝氨酸到天冬酰胺取代的突变是纯合的。他们的杂合父母不受影响,在31例无关的非甲状腺病或正常对照中未发现此突变。与它的位置一致,S57N TTF-2突变蛋白显示受损的DNA结合和部分转录功能丧失。 TTF-2功能的这种不完全丧失可能是由于我们患者中无胆管闭锁和双会厌会导致的,这是在另外两个具有更有害的TTF-2突变的另外两个个体中与CH和c裂共同出现的异常现象( A65V)。我们的观察结果支持TTF-2在甲状腺和上颚发育中的作用,但提示这种CH的症状形式的表型异质性。

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