- Betty Diamond

Abstract

Funding Agency

Agency: National Institute of Health (NIH)
Institute: National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type: Research Project (R01)
Project #: 3R01AR042533-04S1
Application #: 2411427
Study Section: Arthritis and Musculoskeletal and Skin Diseases Special Grants Review Committee (AMS)

Project Start: 1993-12-10
Project End: 1998-11-30
Budget Start: 1996-12-01
Budget End: 1997-11-30
Support Year: 4
Fiscal Year: 1997
Total Cost
Indirect Cost

Institution

Name: Albert Einstein College of Medicine
Department: Microbiology/Immun/Virology
Type: Schools of Medicine
DUNS #: 009095365

City: Bronx
State: NY
Country: United States
Zip Code: 10461

Related projects


NIH 1998 R01 AR	Anti-DNA B-Cell Class II-Mediated Antigen Presentation Diamond, Betty / Albert Einstein College of Medicine
NIH 1998 R01 AR	Antidna B Cell Class II Mediated Antigen Presentation Diamond, Betty / Albert Einstein College of Medicine
NIH 1997 R01 AR	Anti-DNA B-Cell Class II-Mediated Antigen Presentation Diamond, Betty / Albert Einstein College of Medicine
NIH 1997 R01 AR	Diamond, Betty / Albert Einstein College of Medicine
NIH 1996 R01 AR	Anti-DNA B-Cell Class II-Mediated Antigen Presentation Diamond, Betty / Albert Einstein College of Medicine
NIH 1996 R01 AR	Antidna B-Cell Class II Mediated Antigen Presentation Diamond, Betty / Albert Einstein College of Medicine
NIH 1995 R01 AR	Anti-DNA B-Cell Class II-Mediated Antigen Presentation Diamond, Betty / Albert Einstein College of Medicine
NIH 1995 R01 AR	Antidna B-Cell Class II Mediated Antigen Presentation Diamond, Betty / Albert Einstein College of Medicine
NIH 1994 R01 AR	Anti-DNA B-Cell Class II-Mediated Antigen Presentation Diamond, Betty / Albert Einstein College of Medicine

Publications

Kalergis, A M; Boucheron, N; Doucey, M A et al. (2001) Efficient T cell activation requires an optimal dwell-time of interaction between the TCR and the pMHC complex. Nat Immunol 2:229-34

Thomson, C T; Kalergis, A M; Sacchettini, J C et al. (2001) A structural difference limited to one residue of the antigenic peptide can profoundly alter the biological outcome of the TCR-peptide/MHC class I interaction. J Immunol 166:3994-7

Kalergis, A M; Nathenson, S G (2000) Altered peptide ligand-mediated TCR antagonism can be modulated by a change in a single amino acid residue within the CDR3 beta of an MHC class I-restricted TCR. J Immunol 165:280-5

Kuo, P; Bynoe, M S; Wang, C et al. (1999) Bcl-2 leads to expression of anti-DNA B cells but no nephritis: a model for a clinical subset. Eur J Immunol 29:3168-78

Kalergis, A M; Ono, T; Wang, F et al. (1999) Single amino acid replacements in an antigenic peptide are sufficient to alter the TCR V beta repertoire of the responding CD8+ cytotoxic lymphocyte population. J Immunol 162:7263-70

Wang, F; Ono, T; Kalergis, A M et al. (1998) On defining the rules for interactions between the T cell receptor and its ligand: a critical role for a specific amino acid residue of the T cell receptor beta chain. Proc Natl Acad Sci U S A 95:5217-22

Ono, T; DiLorenzo, T P; Wang, F et al. (1998) Alterations in TCR-MHC contacts subsequent to cross-recognition of class I MHC and singly substituted peptide variants. J Immunol 161:5454-63

Spatz, L; Saenko, V; Iliev, A et al. (1997) Light chain usage in anti-double-stranded DNA B cell subsets: role in cell fate determination. J Exp Med 185:1317-26

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