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Thyrotropin internalization is directed by a highly conserved motif in the seventh transmembrane region of its receptor

Authors :
Shi, Yufei
Zou, Minjing
Ahring, Philip
Al-Sedairy, Sultan T.
Farid, Nadir R.
Source :
Endocrine; June 1995, Vol. 3 Issue: 6 p409-414, 6p
Publication Year :
1995

Abstract

The thyrotropin (TSH) receptor is a member of G protein-coupled seven-transmembrane-segment receptors. It is characterized by a large extracellular domain linked to the seven transmembrane segments and ending with a cytoplasmic tail. Sequence alignment shows that a highly conserved motif, NPXXY where X is any amino acid, exists at the boundary between the seventh transmembrane domain and proximal part of the cytoplasmic tail of virtually all G protein-coupled receptors. This motif has been implicated as an internalization signal for several cell surface receptors, such as the low density lipoprotein (LDL), insulin and insulin-like growth factor-1 (IGF-1) receptors. The potential effects of this motif on the TSH receptor signal transduction and receptor-mediated TSH internalization was analysed by replacement of the tyrosine678residue with an alanine residue. This mutation does not impair high affinity TSH binding, but completely abolishes the ability of cAMP response upon TSH stimulation. It also significantly reduces TSH internalization. The role of the cytoplasmic tail of the TSH receptor in receptor-mediated internalization was also assessed. Deletion of up to 56 amino acids from the C-terminus of the cytoplasmic tail enhances TSH internalization as compared to the wild-type receptor. We conclude that tyrosine678in the NPXXY motif is required for efficient receptor-mediated TSH internalization and G protein coupling. The cytoplasmic tail of the TSH receptor may contain sequence domains which could modulate the effects of the NPXXY internalization signal.

Details

Language :
English
ISSN :
1355008x and 15590100
Volume :
3
Issue :
6
Database :
Supplemental Index
Journal :
Endocrine
Publication Type :
Periodical
Accession number :
ejs14801431
Full Text :
https://doi.org/10.1007/BF02935645