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J Biol Chem, Vol. 274, Issue 48, 33979-33984, November 26, 1999
Subunit Structure of Thyrotropin Receptors Expressed on the
Cell Surface
Kunihiko
Tanaka,
Gregorio D.
Chazenbalk,
Sandra M.
McLachlan, and
Basil
Rapoport
From the Autoimmune Disease Unit, Cedars-Sinai Research Institute
and School of Medicine, UCLA, Los Angeles, California 90048
We studied cell surface thyrotropin receptor
(TSHR) by biotinylating proteins on the surface of metabolically
labeled, intact cells. In addition to TSHR cleaved into A and B
subunits, mature single-chain receptors with complex carbohydrate were
also present on the cell surface. A low A/B subunit ratio indicated
partial shedding of extracellular A subunits from transmembrane B
subunits. TSHR cleavage at upstream site 1 (within amino acid residues
305-316) would generate a B subunit of 51-52 kDa. However, only
smaller B subunits (40-46 kDa) were detected, corresponding to N
termini from residues ~370 (site 2) extending downstream to the
region of B subunit insertion into the plasma membrane. The intervening C peptide region between sites 1 and 2 could not be purified from TSHR
epitope-tagged (c-myc) within this region. However, the small proportion of B subunits recovered with a c-myc antibody were larger
(45-52 kDa) than the majority of B subunits recovered with a
C-terminal antibody. In conclusion, our study provides the first characterization of cell surface TSHR including their A and B subunits.
Single-chain, mature TSHR do exist on the cell surface. The C peptide
lost during intramolecular cleavage disintegrates rapidly following
cleavage at upstream site 1 of the single-chain TSHR into A and B
subunits. N-terminal disintegration of the B subunit pauses at site 2, but then progresses downstream to the vicinity of the plasma membrane,
revealing a novel mechanism for A subunit shedding.
Copyright © 1999 by The American Society for Biochemistry and Molecular Biology, Inc.

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Copyright © 1999 by the American Society for Biochemistry and Molecular Biology.
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