Homozygous thyroid hormone receptor β-gene mutations in resistance to thyroid hormone: three new cases and review of the literature
AM Ferrara, K Onigata, O Ercan… - The Journal of …, 2012 - academic.oup.com
AM Ferrara, K Onigata, O Ercan, H Woodhead, RE Weiss, S Refetoff
The Journal of Clinical Endocrinology & Metabolism, 2012•academic.oup.comContext: The most common cause of resistance to thyroid hormone (RTH) is heterozygous
thyroid hormone receptor β (THRB) gene mutations. Homozygous mutations in the THRB
gene are a rare event. Objective: In this study, the clinical findings of three new patients
(belonging to two families) homozygous for mutations in the THRB gene are compared to
three other families in which affected individuals lack a normal TRβ. Methods: We conducted
clinical studies and genetic analyses. Results: The clinical presentation in all three …
thyroid hormone receptor β (THRB) gene mutations. Homozygous mutations in the THRB
gene are a rare event. Objective: In this study, the clinical findings of three new patients
(belonging to two families) homozygous for mutations in the THRB gene are compared to
three other families in which affected individuals lack a normal TRβ. Methods: We conducted
clinical studies and genetic analyses. Results: The clinical presentation in all three …
Context
The most common cause of resistance to thyroid hormone (RTH) is heterozygous thyroid hormone receptor β (THRB) gene mutations. Homozygous mutations in the THRB gene are a rare event.
Objective
In this study, the clinical findings of three new patients (belonging to two families) homozygous for mutations in the THRB gene are compared to three other families in which affected individuals lack a normal TRβ.
Methods
We conducted clinical studies and genetic analyses.
Results
The clinical presentation in all three homozygous subjects was unusually severe; their phenotype was characterized by compromised intellectual development, tachycardia, goiter, growth retardation, and hearing loss. This was comparable with one other reported patient homozygous for mutant TRβ, but not in RTH due to THRB gene deletions.
Conclusion
We report three new subjects, from two families, in whom RTH was associated with homozygous mutations in the THRB gene. They represent an important addition to the single known patient homozygous for a mutant TRβ. The clinical and laboratory abnormalities indicate a strong dominant-negative effect and are in agreement with data obtained from mice expressing a mutant Thrb in both alleles. This report strengthens the concept that the mutated TRβ interferes with the function of the TRα1 in humans.
Oxford University Press