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一名无甲状腺激素受体基因突变的甲状腺激素抵抗患儿:20年随访

A child with resistance to thyroid hormone without thyroid hormone receptor gene mutation: a 20-year follow-up.

作者信息

Hamon Beatrice, Hamon Patrick, Bovier-Lapierre Michel, Pugeat Michel, Savagner Frederique, Rodien Patrice, Orgiazzi Jacques

机构信息

Department of Endocrinology, Centre Hospitalier, Chambéry, France.

出版信息

Thyroid. 2008 Jan;18(1):35-44. doi: 10.1089/thy.2007.0079.

Abstract

We report here the 20-year follow-up study of a male subject diagnosed at 15 months of age as a sporadic case of pituitary resistance to thyroid hormone on the combination of clinical hyperthyroidism, elevated serum thyroid hormone (TH) levels and inappropriate thyrotropin (TSH). On D-thyroxine (D-T(4)) therapy from 30 months of age to 12.5 years, hyperactivity and hyperthyroid signs and symptoms as well as growth abnormalities improved, serum L-thyroxine (L-T(4)) enantiomer normalized, and basal and stimulated TSH decreased significantly without complete suppression. After 8 years off D-T(4), at 20 years of age, clinical status was normal despite persisting high TH levels and inappropriate TSH. Evolution of serum markers of TH action and echocardiography measurements followed up from 15 months to 20 years of age either in basal condition or on triiodothyronine (T(3)), as well as the sequential determination of bone mineral density suggest differences in the tissue responses to T(3): normal in bone with a high remodelling rate, heterogeneity for various hepatic markers, and decreased at heart level. No mutations were found in the coding sequence of TRbeta1, TRbeta2, TRalpha1, RXRgamma, SMRT, NCoR1, and NCoA1. In this patient the putative long-term effects of the persisting high bone resorption are unknown.

摘要

我们在此报告一名男性受试者的20年随访研究,该受试者在15个月大时被诊断为散发性垂体抵抗甲状腺激素,临床表现为甲状腺功能亢进、血清甲状腺激素(TH)水平升高以及促甲状腺激素(TSH)异常。从30个月大到12.5岁接受D-甲状腺素(D-T4)治疗期间,多动、甲状腺功能亢进的体征和症状以及生长异常均有所改善,血清L-甲状腺素(L-T4)对映体恢复正常,基础和刺激后的TSH显著下降但未完全被抑制。停用D-T4 8年后,在20岁时,尽管TH水平持续升高且TSH异常,但临床状态正常。对15个月至20岁期间基础状态或接受三碘甲状腺原氨酸(T3)治疗时TH作用的血清标志物演变及超声心动图测量,以及骨密度的连续测定表明,不同组织对T3的反应存在差异:骨组织反应正常但重塑率高,各种肝脏标志物存在异质性,心脏水平反应降低。在TRbeta1、TRbeta2、TRalpha1、RXRgamma、SMRT、NCoR1和NCoA1的编码序列中未发现突变。在该患者中,持续高骨吸收的潜在长期影响尚不清楚。

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