DOI Page / Citation link:
https://doi.org/10.11588/diglit.48120#0022
4
Molecular and Cell Biology of Autoantibodies and Autoimmunity
DNA elements. In vivo and in vitro structure/function studies using in vitro
engineered mutants and chimeric receptors expressed in animal and yeast cells
have revealed the existence of several functional domains responsible for ligand
binding, nuclear localization, dimerization, DNA binding and activation of
transcription. A model aimed at explaining how nuclear receptors may function
will be discussed.
References
1. Green, S., Chambon, P. (1987): Nature 325, 75
2. Kumar, V. et al. (1987): Cell 51, 941
3. Gronemeyer, H. et al. (1987): EMBO J 6, 3985
4. Petkovich, M. et al. (1987): Nature 330, 444
5. Webster, N. et al. (1988): Cell 52, 169
6. Webster. N. et al. (1988): Cell 54, 199
7. Brand. N. et al. (1988): Nature 332, 850
8. Tora, L. et al. (1988): Nature 333, 185
9. Metzger, D. et al. (1988): Nature 334, 31
10. Green, S. et al. (1988): EMBO J. 7, 3037
11. Kumar, V., Chambon, P. (1988): Cell 55, 145
12. Green, S., Chambon, P. (1988): Trends in Genetics 4, 309
13. Tora, L. et al. (1988): EMBO J. 7, 3771
14. Ponglikitmongkol, M. et al. (1988): EMBO J. 7, 3385
15. Mader, S. et al. (1989): Nature 338, 271
16. Meyer, M. et al. (1989): Cell in press
17. Bocquel, M.T. et al. (1989): Nucl. Acids Res. in press
Multiple Components of SS-A/Ro Autoantigen: cDNA Cloning of the
52kDa Protein
E.K.L. Chan1, J.C. Hamel1, C.L. Peebles1, J.P. Buyon2, and E.M. Tan1
Scripps Clinic and Research Foundation, La Jolla, California, USA
2 Hospital for Joint Diseases Orthopaedic Institute, New York, USA
SS-A/Ro proteins are common autoantibdy targets of patients with Sjogren's
syndrome, systemic lupus, subacute cutaneous lupus, and neonatal lupus. Our
aim is to characterize these components using immunoblotting and cDNA clon-
ing. Human autoimmune SS-A/Ro sere frequently immunoblot a 60 kDa and a
Molecular and Cell Biology of Autoantibodies and Autoimmunity
DNA elements. In vivo and in vitro structure/function studies using in vitro
engineered mutants and chimeric receptors expressed in animal and yeast cells
have revealed the existence of several functional domains responsible for ligand
binding, nuclear localization, dimerization, DNA binding and activation of
transcription. A model aimed at explaining how nuclear receptors may function
will be discussed.
References
1. Green, S., Chambon, P. (1987): Nature 325, 75
2. Kumar, V. et al. (1987): Cell 51, 941
3. Gronemeyer, H. et al. (1987): EMBO J 6, 3985
4. Petkovich, M. et al. (1987): Nature 330, 444
5. Webster, N. et al. (1988): Cell 52, 169
6. Webster. N. et al. (1988): Cell 54, 199
7. Brand. N. et al. (1988): Nature 332, 850
8. Tora, L. et al. (1988): Nature 333, 185
9. Metzger, D. et al. (1988): Nature 334, 31
10. Green, S. et al. (1988): EMBO J. 7, 3037
11. Kumar, V., Chambon, P. (1988): Cell 55, 145
12. Green, S., Chambon, P. (1988): Trends in Genetics 4, 309
13. Tora, L. et al. (1988): EMBO J. 7, 3771
14. Ponglikitmongkol, M. et al. (1988): EMBO J. 7, 3385
15. Mader, S. et al. (1989): Nature 338, 271
16. Meyer, M. et al. (1989): Cell in press
17. Bocquel, M.T. et al. (1989): Nucl. Acids Res. in press
Multiple Components of SS-A/Ro Autoantigen: cDNA Cloning of the
52kDa Protein
E.K.L. Chan1, J.C. Hamel1, C.L. Peebles1, J.P. Buyon2, and E.M. Tan1
Scripps Clinic and Research Foundation, La Jolla, California, USA
2 Hospital for Joint Diseases Orthopaedic Institute, New York, USA
SS-A/Ro proteins are common autoantibdy targets of patients with Sjogren's
syndrome, systemic lupus, subacute cutaneous lupus, and neonatal lupus. Our
aim is to characterize these components using immunoblotting and cDNA clon-
ing. Human autoimmune SS-A/Ro sere frequently immunoblot a 60 kDa and a