Abstract

The objective of this proposal is to define the mechanisms that control lymphocyte trafficking to the small and large intestines, and to characterize their roles in segregating mucosal immune responses and in targeting effector and memory cells to intestinal antigens. 1) The chemoattractant receptors CCR9 and CCR10 and their ligands, the small intestinal epithelial chemokine CCL25, and the widespread mucosal epithelial chemokine CCL28, are well-positioned to control the mucosal recruitment and dissemination of IgA antibody secreting cells (ACS). CCR9, CCR10, and dual receptor-deficient mice will be used to define the role of these receptors in the homeostatic steady-state production and distribution of IgA-secreting cells; to assess their importance in targeting antigen-specific IgA plasma cells responding to intestinal infection; and to examine critically their involvement in the recruitment of circulating IgA ASC from the blood. 2) In a challenge to current concepts of naive T cell trafficking, CDS recent thymic emigrants (RTE) are shown to home directly into the small intestines where they proliferate and differentiate in the intra-epithelial leukocyte (IEL) compartment. The role of CCR9 and CCL25 and other trafficking receptors in CDS RTE recruitment to the intestines will be assessed in homing assays, and thymic single positive mature CDS cells from monospecific T cell receptor transgenic mice will be transferred and monitored to evaluate the importance of mucosal antigen recognition to RTE activation in the gut wall. The ability of RTE to repopulate the epithelial compartment of immunodeficient mice and to contribute to IEL T-cell diversity will be evaluated. These studies have the potential to redefine current understanding of naive cell trafficking, and to identify a key role for thymic T cell export in maintaining a diverse immune repertoire at mucosal surfaces. 3) The homing of colon memory/effector T cells is poorly understood. Flow cytometry-based short term homing assays will be used to identify blast or memory T cell subsets that home well to the normal or inflamed colon, and to seek T cell populations that can home selectively to the colon vs the small intestines. Immunofluorescence and gene microarray studies will identify receptors expressed by colon-homing cells, and homing assays will define the role of these candidate adhesion and chemoattractant receptors in the selectivity of T cell subset recruitment from the blood into intestinal and other sites. Understanding lymphocyte recruitment to normal and inflamed intestines may lead to novel therapeutic approaches in inflammatory bowel diseases, as well as providing insights that can improve methods of vaccination and monitoring of mucosal immunity to HIV and other agents. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI047822-09
Application #
7474662
Study Section
Immunity and Host Defense Study Section (IHD)
Program Officer
Rothermel, Annette L
Project Start
2001-05-01
Project End
2010-07-31
Budget Start
2008-08-01
Budget End
2009-07-31
Support Year
9
Fiscal Year
2008
Total Cost
$333,393
Indirect Cost

  Institution

Name
Palo Alto Institute for Research & Edu, Inc.
Department
Type
DUNS #
624218814
City
Palo Alto
State
CA
Country
United States
Zip Code
94304

  Publications

Bednar, Kyle J; Shanina, Elena; Ballet, Romain et al. (2017) Human CD22 Inhibits Murine B Cell Receptor Activation in a Human CD22 Transgenic Mouse Model. J Immunol 199:3116-3128
Zeng, R; Oderup, C; Yuan, R et al. (2013) Retinoic acid regulates the development of a gut-homing precursor for intestinal dendritic cells. Mucosal Immunol 6:847-56
Hadeiba, Husein; Butcher, Eugene C (2013) Thymus-homing dendritic cells in central tolerance. Eur J Immunol 43:1425-9
Pachynski, Russell K; Zabel, Brian A; Kohrt, Holbrook E et al. (2012) The chemoattractant chemerin suppresses melanoma by recruiting natural killer cell antitumor defenses. J Exp Med 209:1427-35
Nguyen, Tuan M; Ravindra, Dipti; Kwong, Brian et al. (2012) Differential expression of alpha 4 integrins on effector memory T helper cells during Bordetella infections. Delayed responses in Bordetella pertussis. PLoS One 7:e52903
Huss, Ryan S; Huddleston, James I; Goodman, Stuart B et al. (2010) Synovial tissue-infiltrating natural killer cells in osteoarthritis and periprosthetic inflammation. Arthritis Rheum 62:3799-805
Zúñiga, Luis A; Shen, Wen-Jun; Joyce-Shaikh, Barbara et al. (2010) IL-17 regulates adipogenesis, glucose homeostasis, and obesity. J Immunol 185:6947-59
Brown, Meghan N; Fintushel, Sarah R; Lee, Michael H et al. (2010) Chemoattractant receptors and lymphocyte egress from extralymphoid tissue: changing requirements during the course of inflammation. J Immunol 185:4873-82
Graham, Kareem L; Zabel, Brian A; Loghavi, Sanam et al. (2009) Chemokine-like receptor-1 expression by central nervous system-infiltrating leukocytes and involvement in a model of autoimmune demyelinating disease. J Immunol 183:6717-23
Lin, Francis; Butcher, Eugene C (2008) Modeling the role of homologous receptor desensitization in cell gradient sensing. J Immunol 181:8335-43

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