生殖系促甲状腺激素受体激活突变相关甲状腺功能亢进症的基因型-表型相关性:一项系统评价
Genotype-Phenotype Correlation in Germline TSH Receptor Activating Mutation Associated Hyperthyroidism: A Systematic Review.
作者信息
Yamichannaiah Chethan, Memon Saba Samad, Sarathi Vijaya, Lila Anurag Ranjan, Jadhav Swati Ramteke, Thadani Puja, Hegishte Samiksha Chandrashekhar, Barnabas Rohit, Karlekar Manjiri, Phadte Aditya, Sharma Anima, Bandgar Tushar
机构信息
Department of Endocrinology, Seth GS Medical College and KEM Hospital, Parel, Mumbai, India.
Department of Endocrinology, Vydehi Institute of Medical Sciences and Research Centre, Bengaluru, India.
出版信息
Clin Endocrinol (Oxf). 2025 Aug;103(2):119-128. doi: 10.1111/cen.15288. Epub 2025 Jun 5.
OBJECTIVE
Germline TSHR activating mutation-associated hyperthyroidism (GTAMH) manifests as sporadic or familial forms. Studies have shown poor correlation between receptor activity and clinical manifestations, highlighting a knowledge gap in understanding genotype-phenotype relationships.
DESIGN
A classification based on age of symptom onset: infantile (n = 36), childhood (n = 33) and adulthood (> 18 years, n = 13) was attempted by performing a systematic review of literature of GTAMH (n = 82 probands, including a 25-year-old woman with TSHR p.Ile640Val variant and subclinical hyperthyroidism managed at our centre). Patients were analysed for various parameters such as demographic, clinical, biochemical and genotype-phenotype correlation.
RESULTS
Eighty-two probands harbouring 47 different TSHR variants are reported. Probands with infantile-onset were less often familial (19.4%, p = 0.00) than childhood (93.9%) and adult-onset (84.6%) cases. Median serum free-T3 and T4 were highest in infantile (3.1 and 3.4 XULN) followed by childhood (1.6 and 1.9 X-ULN) and adult-onset (1.2 and 0.8 X-ULN) cases. All infant/childhood onset probands had overt hyperthyroidism, whereas 1/3 of adult-onset cases were subclinical. Most (15/18) recurrent variants were exclusive to infantile, childhood or adult-onset disease groups, except for p.Ser505Asn, p.Asp619Gly and p.Asn670Ser. Including data for probands and genetically affected family members, there was a moderate correlation for the age at diagnosis (infancy, childhood or adulthood), among family members (r = 0.40, p = 0.00), and members of multiple families harbouring the same TSHR variants (r = 0.46, p = 0.00).
CONCLUSION
A phenotypic classification of GTAMH into infantile-onset severe hyperthyroxinemia (mostly due to de novo variants), childhood-onset overt hyperthyroidism or adulthood-onset overt/subclinical hyperthyroidism correlates with the genotype of TSHR variants, may guide patient management.
目的
胚系促甲状腺激素受体(TSHR)激活突变相关的甲状腺功能亢进症(GTAMH)表现为散发性或家族性形式。研究表明受体活性与临床表现之间的相关性较差,这突出了在理解基因型-表型关系方面的知识空白。
设计
通过对GTAMH文献(n = 82名先证者,包括一名在我们中心接受治疗的患有TSHR p.Ile640Val变异和亚临床甲状腺功能亢进症的25岁女性)进行系统回顾,尝试根据症状出现年龄进行分类:婴儿期(n = 36)、儿童期(n = 33)和成年期(> 18岁,n = 13)。对患者的各种参数进行分析,如人口统计学、临床、生化和基因型-表型相关性。
结果
报告了82名携带47种不同TSHR变异的先证者。婴儿期发病的先证者家族性的比例(19.4%,p = 0.00)低于儿童期(93.9%)和成年期发病(84.6%)的病例。婴儿期血清游离T3和T4中位数最高(3.1和3.4倍正常上限),其次是儿童期(1.6和1.9倍正常上限)和成年期发病(1.2和0.8倍正常上限)的病例。所有婴儿/儿童期发病的先证者均为显性甲状腺功能亢进症,但成年期发病病例中有1/3为亚临床型。除了p.Ser505Asn、p.Asp619Gly和p.Asn670Ser外,大多数(15/18)复发变异仅见于婴儿期、儿童期或成年期发病的疾病组。纳入先证者和遗传受累家庭成员的数据后,在家庭成员之间(r = 0.40, p = 0.00)以及携带相同TSHR变异的多个家庭的成员之间(r = 0.46, p = 0.00),诊断年龄(婴儿期、儿童期或成年期)存在中度相关性。
结论
将GTAMH表型分类为婴儿期发病的严重高甲状腺素血症(主要由于新发变异)、儿童期发病的显性甲状腺功能亢进症或成年期发病的显性/亚临床甲状腺功能亢进症与TSHR变异的基因型相关,可能指导患者管理。
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