Abstract

The objective of this training program high quality pre- and postdoctoral training in immunology and molecular pathogenesis to highly qualified candidates. The rationale for the program includes the importance of interdisciplinary training in providing the foundation for investigating mechanisms of pathogenesis, the recent recruitment to Emory of a large number of investigators that has resulted in a major expansion in the participating faculty, the extensive previous involvement of the participating faculty in pre- and postdoctoral training and the expanding opportunities for research in the areas represented by jthis program. The faculty in the graduate Program in Immunology and Molecular Pathogenesis (IMP) have the expertise required to provide the foundation that is critical for outstanding predoctoral and postdoctoral training. Many of the participating faculty have extensive training records, in some cases initiated at their former institutions prior to their recruitment to Emory. The areas of research represented by this program have outstanding potential for future investigations and for providing new insights into disease pathogenesis. Utilizing multiple experimental approaches in immunobiology, molecular and cell biology, pathobiology, and genetics, the research programs of the faculty members fall into 4 main training areas: 1) pathogenesis of infectious diseases; 2) molecular genetics of the immune system; 3) cell biology and oncogenesis; and 4) immunobiology. The faculty are members of 4 basic science or clinical departments in the School of Medicine. Therefore, the interdisciplinary approach to the investigation of disease mechanisms will be fostered by this program. Extensive interactions of the program faculty, including: collaborative research projects, joint research group meetings, joint weekly seminars, and joint participation in the Immunology and Molecular Pathogenesis (IMP) Graduate Program will enhance the interdisciplinary training of the candidates appointed to this program. ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Institutional National Research Service Award (T32)
Project #
2T32AI007610-06
Application #
6948995
Study Section
Allergy & Clinical Immunology-1 (AITC)
Program Officer
Prograis, Lawrence J
Project Start
2000-09-01
Project End
2010-08-31
Budget Start
2005-09-01
Budget End
2006-08-31
Support Year
6
Fiscal Year
2005
Total Cost
$373,979
Indirect Cost

  Institution

Name
Emory University
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
066469933
City
Atlanta
State
GA
Country
United States
Zip Code
30322

  Publications

Laurie, Sonia J; Liu, Danya; Wagener, Maylene E et al. (2018) 2B4 Mediates Inhibition of CD8+ T Cell Responses via Attenuation of Glycolysis and Cell Division. J Immunol 201:1536-1548
McMaster, Sean R; Wein, Alexander N; Dunbar, Paul R et al. (2018) Pulmonary antigen encounter regulates the establishment of tissue-resident CD8 memory T cells in the lung airways and parenchyma. Mucosal Immunol 11:1071-1078
Andargachew, Rakieb; Martinez, Ryan J; Kolawole, Elizabeth M et al. (2018) CD4 T Cell Affinity Diversity Is Equally Maintained during Acute and Chronic Infection. J Immunol 201:19-30
Barwick, Benjamin G; Scharer, Christopher D; Martinez, Ryan J et al. (2018) B cell activation and plasma cell differentiation are inhibited by de novo DNA methylation. Nat Commun 9:1900
Bally, Alexander P R; Tang, Yan; Lee, Joshua T et al. (2017) Conserved Region C Functions To Regulate PD-1 Expression and Subsequent CD8 T Cell Memory. J Immunol 198:205-217
Shwetank; Abdelsamed, Hossam A; Frost, Elizabeth L et al. (2017) Maintenance of PD-1 on brain-resident memory CD8 T cells is antigen independent. Immunol Cell Biol 95:953-959
Scharer, Christopher D; Bally, Alexander P R; Gandham, Bhanu et al. (2017) Cutting Edge: Chromatin Accessibility Programs CD8 T Cell Memory. J Immunol 198:2238-2243
Cook, D A; Kannarkat, G T; Cintron, A F et al. (2017) LRRK2 levels in immune cells are increased in Parkinson's disease. NPJ Parkinsons Dis 3:11
Liu, Yang; Blanchfield, Lori; Ma, Victor Pui-Yan et al. (2016) DNA-based nanoparticle tension sensors reveal that T-cell receptors transmit defined pN forces to their antigens for enhanced fidelity. Proc Natl Acad Sci U S A 113:5610-5
Shorter, Shayla K; Schnell, Frederick J; McMaster, Sean R et al. (2016) Viral Escape Mutant Epitope Maintains TCR Affinity for Antigen yet Curtails CD8 T Cell Responses. PLoS One 11:e0149582

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