Details Of Published TSH Receptor Mutation
Ile 486 Phe
c.1457T>AConstitutively Activating TSH Receptor Mutation
Type
gain
Manifestation
carcinoma
Exon
10
Molecular Characteristics:
default
Clinical Features:
follicular carcinoma with clinical phenotype of "hot nodule"
* based on 13 hot nodules investigated by Parma et al. 1995 and 1997, TrĆ¼lzsch et al. 2001, Van Sande et al. 1995, Tonacchera et al. 2000, Gozu et al. 2006, Paloz-Paz et al. 2008 and Georgopulos et al. 2003
and 2 hot thyroid carcinomas investigated by Camacho et al. 2000 and Bircan et al. 2005
* based on 13 hot nodules investigated by Parma et al. 1995 and 1997, TrĆ¼lzsch et al. 2001, Van Sande et al. 1995, Tonacchera et al. 2000, Gozu et al. 2006, Paloz-Paz et al. 2008 and Georgopulos et al. 2003
and 2 hot thyroid carcinomas investigated by Camacho et al. 2000 and Bircan et al. 2005
Treatment:
default
Functional Characteristics:
cAMP
(basal)
(basal)
cAMP
(TSH)
(TSH)
IP
(basal)
(basal)
IP
(TSH)
(TSH)
TSH-Binding
Cell Surface Expression
Prevalence
LRA
Ref
4.0-8.2
0.8
1.0-3.3
0.4
-
0.2-0.4
2
57.8+/-6.9
1,2,5,6
Legend:
cAMP (basal): basal in vitro cAMP production of mutant over wild-type TSHR
cAMP (TSH): maximal in vitro cAMP production of mutant over wild-type TSHR
IP (basal): basal in vitro IP production of mutant over wild-type TSHR
IP (TSH): maximal in vitro IP production of mutant over wild-type TSHR
TSH-binding: maximal TSH-binding compared to the wild-type TSHR
Cell surface expression: cell surface expression of mutant compared to WT-TSHR
LRA: linear regression analysis (LRA) of constitutive activity as a function of TSHR expression determined by 125I-bTSH binding or FACS analysis compared to the wild-type TSHR
Prevalence: Prevalence of (somatic and germline) activating mutations*
Ref: Reference for functional characterization
Child: Found in children.
Reference 1:
Parma et al.
Mol. Endocrinol. 9: 725-733
Somatic mutations causing constitutive activity of the thyrotropin receptor are the major cause of hyperfunctioning thyroid adenomas: identification of additional mutations activating both the cyclic adenosine 3',5'-monophosphate and inositol phosphate-Ca
1995
Reference 2:
Claeysen et al.
FEBS Lett 517: 195-200
A conserved Asn in TM7 of the thyrotropin receptor is a common requirement for activation by both mutations and its natural agonist.
2002
Reference 3:
Camacho et al.
Thyroid 10: 1009-1012
A Phe 486 thyrotropin receptor mutation in an autonomously functioning follicular carcinoma that was causing hyperthyroidism.
2000
Reference 4:
Bircan et al.
Abstract Book 32nd Annual Meeting of the European Thyroid Association, 01.-05.09.2007 Leipzig.
The Second Follicular Thyroid Carcinoma Presenting as a Hot Nodule with a Somatic I486F TSH-Receptor (TSHR) Gene Mutation
2005
Reference 5:
Ho et al.
Mol Cell Endocrinol 245:158-168
Cysteine 390 mutation of the TSH receptor modulates its ectodomain as an inverse agonist on the serpentine domain with decrease in basal constitutive activity.
2005
Reference 6:
Neumann et al.
Eur J Endocrinol 152:625-634
Interactions between the extracellular domain and the extracellular loops as well as the 6th transmembrane domain are necessary for TSH receptor activation.
2005