Abstract

A proper immune response requires a well-orchestrated interaction among rare antigen-specific lymphocytes and antigen presenting cells, both temporally and spatially. The highly organized lymphoid tissues, lymph nodes (LN) or Peyer's patches (PP), may provide such proper micro- environment. However, the essential components for the development and function of these lymphoid tissues have not been well elucidated. Mice congenitally deficient of lymphotoxin-alpha (LTalpha) manifest impaired splenic architecture and no LN or PP. It appears that the defect in lymphoid structures without intrinsic defect of lymphocytes in LTalpha- /- mice leads to impaired immune responses. It is suggested that the development of splenic microenvironment is regulated by LTalpha- expressing B cells while the organogenesis of LN and PP is mediated by LTalpha-expressing non-T and non-B cells. We will study 1) the regulatory mechanisms of prenatal organogenesis of lymphoid tissues and 2) the consequences of defective peripheral lymphoid tissues in immune responses. To determine whether NK cells, non-T and non-B cells, play an essential role in the formation of lymphoid s*tructures, either reconstitution of LTalpha-/- mice with LT-expressing NK cells or blockage of the function of these cells in normal mice will be performed before or after birth. Furthermore, various immunodeficient mouse models with selected deficiency in either LN, or PP, or different form of LT can be generated by regulating LT activity to the different stage of development. The ability of these mouse models to generate systemic immune response to localized antigens will be subsequently explored to better dissect the functions of individual lymphoid structure or different form of LT. The cellular responses to local antigens in draining LN and the role of PP in gut-associated immunity can be better elucidated. More complete understanding of the development and function of these lymphoid tissues may help us to elucidate the mechanisms of various immunodeficient diseases associated with the defects of lymphoid tissues and provide new approaches for manipulation of immune responses and management of immunocompromised hosts.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD037104-02
Application #
6181814
Study Section
Immunobiology Study Section (IMB)
Program Officer
Lock, Allan
Project Start
1999-04-06
Project End
2004-03-31
Budget Start
2000-04-01
Budget End
2001-03-31
Support Year
2
Fiscal Year
2000
Total Cost
$98,685
Indirect Cost

  Institution

Name
University of Chicago
Department
Pathology
Type
Schools of Medicine
DUNS #
225410919
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Yu, Ping; Lee, Youjin; Wang, Yang et al. (2007) Targeting the primary tumor to generate CTL for the effective eradication of spontaneous metastases. J Immunol 179:1960-8
Wang, Jing; Anders, Robert A; Wang, Yang et al. (2005) The critical role of LIGHT in promoting intestinal inflammation and Crohn's disease. J Immunol 174:8173-82
Yu, Ping; Lee, Youjin; Liu, Wenhua et al. (2005) Intratumor depletion of CD4+ cells unmasks tumor immunogenicity leading to the rejection of late-stage tumors. J Exp Med 201:779-91
Wang, Jing; Fu, Yang-Xin (2005) Tumor necrosis factor family members and inflammatory bowel disease. Immunol Rev 204:144-55
Subudhi, Sumit K; Zhou, Ping; Yerian, Lisa M et al. (2004) Local expression of B7-H1 promotes organ-specific autoimmunity and transplant rejection. J Clin Invest 113:694-700
Yu, Ping; Lee, Youjin; Liu, Wenhua et al. (2004) Priming of naive T cells inside tumors leads to eradication of established tumors. Nat Immunol 5:141-9
Chin, Robert; Wang, Jing; Fu, Yang-Xin (2003) Lymphoid microenvironment in the gut for immunoglobulin A and inflammation. Immunol Rev 195:190-201
Yu, Ping; Spiotto, Michael T; Lee, Youjin et al. (2003) Complementary role of CD4+ T cells and secondary lymphoid tissues for cross-presentation of tumor antigen to CD8+ T cells. J Exp Med 197:985-95
Wang, Y; Huang, G; Wang, J et al. (2000) Antigen persistence is required for somatic mutation and affinity maturation of immunoglobulin. Eur J Immunol 30:2226-34