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毒性多结节性甲状腺肿患者亚群中组成性激活的体细胞促甲状腺素受体突变的鉴定。

Identification of constitutively activating somatic thyrotropin receptor mutations in a subset of toxic multinodular goiters.

作者信息

Holzapfel H P, Führer D, Wonerow P, Weinland G, Scherbaum W A, Paschke R

机构信息

Department of Internal Medicine III, University of Leipzig, Germany.

出版信息

J Clin Endocrinol Metab. 1997 Dec;82(12):4229-33. doi: 10.1210/jcem.82.12.4441.

Abstract

Constitutively activating mutations in the TSH receptor (TSHR) gene and in the Gs alpha gene are frequent molecular causes for solitary toxic nodules of the thyroid. However, the etiology of toxic multinodular goiter is still largely unknown. Therefore, DNA from nodular and quiescent surrounding tissue of six patients with toxic multinodular goiters was screened for mutations in exons 9 and 10 of the TSHR gene and exons 7-10 of the Gs alpha gene by direct automated sequencing. In one patient, two different somatic TSHR mutations were identified in two different toxic nodules (L632I and F631L). In another patient, two different toxic nodules harbored the same TSHR mutation (I630L), whereas only one TSHR mutation (F631L) was identified in one of the two toxic nodules of an additional patient. In the other three patients, no mutations could be found in exons 9 and 10 of the TSHR gene or in exons 7-10 of the Gs alpha gene. Our results demonstrate that not only solitary toxic adenomas but also toxic multinodular goiters can be caused by constitutively activating mutations of the TSHR. In addition to mutations in the TSHR and possibly in Gs alpha, there are probably other still unknown mechanisms that cause hot nodules in toxic multinodular goiters.

摘要

促甲状腺激素受体(TSHR)基因和Gsα基因的组成性激活突变是甲状腺单发毒性结节常见的分子病因。然而,毒性多结节性甲状腺肿的病因仍大多不明。因此,通过直接自动测序对6例毒性多结节性甲状腺肿患者的结节及周围静止组织的DNA进行TSHR基因第9和10外显子以及Gsα基因第7 - 10外显子的突变筛查。在1例患者中,在两个不同的毒性结节中鉴定出两种不同的体细胞TSHR突变(L632I和F631L)。在另1例患者中,两个不同的毒性结节存在相同的TSHR突变(I630L),而在另1例患者的两个毒性结节中的1个结节中仅鉴定出1种TSHR突变(F631L)。在其他3例患者中,未在TSHR基因的第9和10外显子或Gsα基因的第7 - 10外显子中发现突变。我们的结果表明,不仅单发毒性腺瘤,而且毒性多结节性甲状腺肿也可由TSHR的组成性激活突变引起。除了TSHR以及可能的Gsα突变外,可能还有其他仍未知的机制导致毒性多结节性甲状腺肿中的热结节。

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