Abstract

The goal of this grant proposal is to further our understanding of the structure and pathophysiologic function of the human TSH receptor (TSHR). We will address the following specific issues:-1. Cleavage of the TSHR: Recent evidence suggests that the large TSHR ectodomain contains two cleavage sites not one as previously thought. We plan to:- (l) Localize the two cleavage sites; (ii) Purify and characterize the putative TSHR C peptide released by intramolecular cleavage; (iii) Determine whether TSHR cleavage occurs in the Golgi complex or after trafficking to the plasma membrane; (iv) Test the hypothesis that TSHR cleavage plays a role in receptor turnover. 2. Overexpression of the TSHR in mammalian cells: Recently, we succeeded in overexpressing the wild-type TSHR in Chinese hamster ovary cells. To provide material for further studies on TSHR cleavage, to stud autoantibody and human TSH interaction with the TSHR, as well as to crystallize a portion of the TSHR ectodomain we wish to attain high level expression of several TSHR variants, including:- (i) a TSHR with a c-myc epitope within the C peptide; (ii) a TSHR cleavage knockout; (iii) Flag epitope-tagged holoreceptors; (iv) Signal transduction deficient holoreceptors; (v) Chimeric TSH-LH/CG receptors selected for their value in discriminating among different types C autoantibodies; (vii) Secreted, soluble TSHR ectodomain variants with 6H epitope tags. 3. Autoantibody and human TSH interaction with the TSHR: We will:- (l) establish direct TSHR autoantibody binding assays using different forms of the TSHR; (ii) complete our mutagenesis studies to localize the region(s) C difference between the human and bovine TSH binding sites on the human TSHR; (iii) explore the role of specie (both ligand and receptor) in assays for TSHR autoantibodies. 4. Role of the 3' untranslated region (UTR) In TSHR expression: The human TSHR 3'UTR plays a major role in suppressing the level of TSHR expression in CHO cells. We propose to examine if the 3'UTR plays a similar role in thyrocytes, to localize the region related to mRNA destabilization, and to investigate putative trans-acting factors that interact with the 3'UTR segment associated with TSHR mRNA destabilization. A similar mechanism in thyroid cells might explain, in part. the very small number of TSHR expressed in thyroid tissue; Also, potential mutations this re ion, b influencing the level of TSHR expression could influence thyroid function.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK019289-25
Application #
6176556
Study Section
Endocrinology Study Section (END)
Program Officer
Akolkar, Beena
Project Start
1976-05-01
Project End
2002-06-30
Budget Start
2000-07-01
Budget End
2001-06-30
Support Year
25
Fiscal Year
2000
Total Cost
$402,153
Indirect Cost

  Institution

Name
Cedars-Sinai Medical Center
Department
Type
DUNS #
075307785
City
Los Angeles
State
CA
Country
United States
Zip Code
90048

  Publications

McLachlan, Sandra M; Lesage, Sylvie; Collin, Roxanne et al. (2017) Genes Outside the Major Histocompatibility Complex Locus Are Linked to the Development of Thyroid Autoantibodies and Thyroiditis in NOD.H2h4 Mice. Endocrinology 158:702-713
Ludwig, Ralf J; Vanhoorelbeke, Karen; Leypoldt, Frank et al. (2017) Mechanisms of Autoantibody-Induced Pathology. Front Immunol 8:603
McLachlan, Sandra M; Aliesky, Holly; Banuelos, Bianca et al. (2017) Variable Effects of Dietary Selenium in Mice That Spontaneously Develop a Spectrum of Thyroid Autoantibodies. Endocrinology 158:3754-3764
Rapoport, Basil; Banuelos, Bianca; Aliesky, Holly A et al. (2016) Critical Differences between Induced and Spontaneous Mouse Models of Graves' Disease with Implications for Antigen-Specific Immunotherapy in Humans. J Immunol 197:4560-4568
Rapoport, Basil; McLachlan, Sandra M (2016) TSH Receptor Cleavage Into Subunits and Shedding of the A-Subunit; A Molecular and Clinical Perspective. Endocr Rev 37:114-34
Rapoport, Basil; McLachlan, Sandra M (2016) TSH Receptor Cleavage Into Subunits and Shedding of the A-Subunit; A Molecular and Clinical Perspective. Endocr Rev 2016:23-42
Chen, Chun-Rong; Salazar, Larry M; McLachlan, Sandra M et al. (2015) Deleting the Redundant TSH Receptor C-Peptide Region Permits Generation of the Conformationally Intact Extracellular Domain by Insect Cells. Endocrinology 156:2732-8
Rapoport, Basil; Aliesky, Holly A; Chen, Chun-Rong et al. (2015) Evidence that TSH Receptor A-Subunit Multimers, Not Monomers, Drive Antibody Affinity Maturation in Graves' Disease. J Clin Endocrinol Metab 100:E871-5
Chen, Chun-Rong; Hubbard, Paul A; Salazar, Larry M et al. (2015) Crystal structure of a TSH receptor monoclonal antibody: insight into Graves' disease pathogenesis. Mol Endocrinol 29:99-107
Rapoport, Basil; Aliesky, Holly A; Banuelos, Bianca et al. (2015) A unique mouse strain that develops spontaneous, iodine-accelerated, pathogenic antibodies to the human thyrotrophin receptor. J Immunol 194:4154-61

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