Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UNIPROT:Q9UIJ5 (
Rec
)
58,342
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
We have assessed the regulatory influence of human recombinant TSH (rec-hTSH) on its homologous receptor (
TSHR
) using a well characterized human fetal thyroid monolayer cell culture technique. Under the culture conditions employed, fetal human thyroid cells showed basal expression of
TSHR
-specific mRNA transcripts, and the addition of
rec
-hTSH (1 U/L) induced up to an 8-fold increase in specific mRNA over a 48-h observation period. This induction was simulated by bromo-cAMP in a dose-dependent manner, indicating that the stimulatory effect of
rec
-hTSH was active at the postreceptor level. Furthermore, there was no detectable increase in the transcription rate of the
TSHR
gene after stimulation with
rec
-hTSH for 12-36 h, although a marked increase in thyroglobulin-specific mRNA was observed.
Rec
-hTSH also had no influence on the half-life of
TSHR
-specific mRNA, which remained at approximately 16 h in the presence or absence of
rec
-hTSH. These data indicate that
rec
-hTSH induced up-regulation in human thyroid cell
TSHR
-specific mRNA and that the mechanism of this regulation was likely to be secondary to a posttranscriptional nuclear event involving changes in the regulation of primary unspliced mRNA for the
TSHR
.
...
PMID:The positive regulation of human thyrotropin (TSH) receptor messenger ribonucleic acid by recombinant human TSH is at the intranuclear level. 157 98
Twenty-two subjects in a family with Graves' Disease and 20 normal subjects unrelated to the family were examined for T-cell responses to
rec
h
TSHR
-ECD and its synthetic peptides. Seven of the family members and none of the controls responded positively to
rec
h
TSHR
-ECD. Peptide 158-176 was the only residue that showed a high percentage of response among family members, no responses in spouses, and a significant difference compared to unrelated controls. Family members under age of 6 did not differ from spouses in response to
rec
h
TSHR
-ECD or any individual peptide. Family members ages 6-12 years were significantly different from spouses in response to peptides 30-49, 158-176, and 172-186. The reactivity of adult family members including 3 Graves' patients was significantly different from spouses in response to peptides 44-62, 132-150, 158-176, and 248-263. The responses of female members of the family were higher than that of the male members and significantly different for peptide 272-291. These data suggest that recognition of peptide 158-176 may be an early event in the pathogenesis of the disease and that recognition of both 158-176 and 248-263 residues may be the cornerstone for establishment of the disease.
...
PMID:T-cell recognition of residue 158-176 in thyrotropin receptor confers risk for development of thyroid autoimmunity in siblings in a family with Graves' disease. 900 Nov 88
