Abstract

Phenotypically distinct populations of thymic epithelial cells (TE) support different aspects of thymocyte development, with cortical TE contributing to prothymocyte expansion and positive selection, and medullary TE participating in negative selection. The basis for this TE heterogeneity, the interactions that mediate the establishment these functional and morphologically distinct epithelial compartments are ill-defined and the nature of their interactions with thymocytes remain poorly understood. Studies proposed here will examine two related aspects of the thymic environment and cortical TE in particular. The first is concerned with the cellular mechanisms involved in thymus organogenesis involving the interactions between epithelial cells and between epithelial cells and immigrant T cell progenitors which lead to the development of the cortical thymic environment. In vitro models of thymus organogenesis will examine the involvement of selected adhession molecules in the establishment of a functional TE compartment with particular emphasis on the cortical TE population and the differentiation potential of T cell progenitors. The second is directed at understanding the role of cortical TE in positive selection and other poximal aspects of thymocyte development. In these studies, advantage will be taken of novel cellular reagents which phenotypically and functionally resemble cortical TE and are used in an in vitro co-culture system to reproduce some aspects of cortical TE function in vitro. This in vitro approach to thymocyte development will be used to define the TE cell surface molecules and soluble products that affect T cell development. As part of this effort, the functional properties of a novel cytokine produced by these TE cells will be further characterized and basic information regarding the expression pattern of this cytokine and it's receptor will be determined. Understanding the interplay between thymocyte and TE that regulate the development and maintenance of the lymphopoietic environment has important clinical relevance and may lead to therapeutic modalities that would be beneficial in reversing the effects of primary or acquired immunodeficiencies affecting T cell production and may be useful in designing approaches to retard age-related loss of thymic function. Defining the molecules and cell interactions that regulate normal lymphocyte development also provides the knowledge necessary for an understanding of the dysregulation of these processes that contribute to autoimmune disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI024137-12
Application #
2882133
Study Section
Immunobiology Study Section (IMB)
Program Officer
Quill, Helen R
Project Start
1986-12-01
Project End
2000-05-31
Budget Start
1999-03-01
Budget End
2000-05-31
Support Year
12
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Washington
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
135646524
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Liston, Adrian; Nutsch, Katherine M; Farr, Andrew G et al. (2008) Differentiation of regulatory Foxp3+ T cells in the thymic cortex. Proc Natl Acad Sci U S A 105:11903-8
Dooley, James; Erickson, Matthew; Larochelle, William J et al. (2007) FGFR2IIIb signaling regulates thymic epithelial differentiation. Dev Dyn 236:3459-71
Gillard, Geoffrey O; Dooley, James; Erickson, Matthew et al. (2007) Aire-dependent alterations in medullary thymic epithelium indicate a role for Aire in thymic epithelial differentiation. J Immunol 178:3007-15
Dooley, James; Erickson, Matthew; Gillard, Geoffrey O et al. (2006) Cervical thymus in the mouse. J Immunol 176:6484-90
Gillard, Geoffrey O; Farr, Andrew G (2006) Features of medullary thymic epithelium implicate postnatal development in maintaining epithelial heterogeneity and tissue-restricted antigen expression. J Immunol 176:5815-24
Fontenot, Jason D; Dooley, James L; Farr, Andrew G et al. (2005) Developmental regulation of Foxp3 expression during ontogeny. J Exp Med 202:901-6
Rodriguez-Galan, Maria Cecilia; Bream, Jay H; Farr, Andrew et al. (2005) Synergistic effect of IL-2, IL-12, and IL-18 on thymocyte apoptosis and Th1/Th2 cytokine expression. J Immunol 174:2796-804
Dooley, James; Erickson, Matt; Farr, Andrew G (2005) An organized medullary epithelial structure in the normal thymus expresses molecules of respiratory epithelium and resembles the epithelial thymic rudiment of nude mice. J Immunol 175:4331-7
Dooley, James; Erickson, Matthew; Roelink, Henk et al. (2005) Nude thymic rudiment lacking functional foxn1 resembles respiratory epithelium. Dev Dyn 233:1605-12
Cooper, Cristine J; Turk, Gail L; Sun, Mingyi et al. (2004) Cutting edge: TCR revision occurs in germinal centers. J Immunol 173:6532-6

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