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Research Article Free access | 10.1172/JCI116233

An arginine to histidine mutation in codon 311 of the C-erbA beta gene results in a mutant thyroid hormone receptor that does not mediate a dominant negative phenotype.

M E Geffner, F Su, N S Ross, J M Hershman, C Van Dop, J B Menke, E Hao, R K Stanzak, T Eaton, and H H Samuels

Department of Pediatrics, UCLA Medical Center 90024.

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Department of Pediatrics, UCLA Medical Center 90024.

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Department of Pediatrics, UCLA Medical Center 90024.

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Department of Pediatrics, UCLA Medical Center 90024.

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Department of Pediatrics, UCLA Medical Center 90024.

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Department of Pediatrics, UCLA Medical Center 90024.

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Department of Pediatrics, UCLA Medical Center 90024.

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Department of Pediatrics, UCLA Medical Center 90024.

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Published February 1, 1993 - More info

Published in Volume 91, Issue 2 on February 1, 1993
J Clin Invest. 1993;91(2):538–546. https://doi.org/10.1172/JCI116233.
© 1993 The American Society for Clinical Investigation
Published February 1, 1993 - Version history
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Abstract

We have examined the c-erbA beta thyroid hormone receptor gene in a kindred, G.H., with a member, patient G.H., who had a severe form of selective pituitary resistance to thyroid hormones (PRTH). This patient manifested inappropriately normal thyrotropin-stimulating hormone, markedly elevated serum free thyroxine (T4) and total triiodothyronine (T3), and clinical hyperthyroidism. The complete c-erbA beta 1 coding sequence was examined by a combination of genomic and cDNA cloning for patient G.H. and her unaffected father. A single mutation, a guanine to adenine transition at nucleotide 1,232, was found in one allele of both these members, altering codon 311 from arginine to histidine. In addition, a half-sister of patient G.H. also harbored this mutant allele and, like the father, was clinically normal. The G.H. receptor, synthesized with reticulocyte lysate, had significantly defective T3-binding activity with a Ka of approximately 5 x 10(8) M-1. RNA phenotyping using leukocytes and fibroblasts demonstrated an equal level of expression of wild-type and mutant alleles in patient G.H. and her unaffected father. Finally, the G.H. receptor had no detectable dominant negative activity in a transfection assay. Thus, in contrast to the many other beta-receptor mutants responsible for the generalized form of thyroid hormone resistance, the G.H. receptor appeared unable to antagonize normal receptor function. These results suggest that the arginine at codon 311 in c-erbA beta is crucial for the structural integrity required for dominant negative function. The ARG-311-HIS mutation may contribute to PRTH in patient G.H. by inactivating a beta-receptor allele, but it cannot be the sole cause of the disease.

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