Abstract

The development and establishment of the B cell repertoire is the net result of both genetic environmental forces. The primary event at the genetic level is Ig gene rearrangement resulting in numerous possible combinations of genes which can be further modified by somatic events such as N segment addition and somatic mutations. Environmental forces in the form of self and exogenous Ags also shape the repertoire by positively or negatively selecting B cells according to the specificity of their Ig receptors. These are dynamic processes beginning with the earliest expression of immunoglobulins in fetal life and continuing throughout life. These studies will analyze the early repertoires in mice with the goal of determining genetic and selective mechanisms responsible for differences in the early immune system compared to that of the adult. Mechanisms responsible for the self-reactivity, polyreactivity and connectivity which characterize the fetal and neonatal repertoire will be determined in B cells. Immunoglobulin transgenic mouse models will be used to define the antigens involved in the selection process, to determine the phenotypes of B cells at different stages of differentiation and selection, and seek out the fetal and anatomical sites where positive and negative selection of B cells occurs. These studies will include a global analysis of the early repertoire with respect to the idiotype/anti- idiotype interactions that occur early in development. The impact of Tdt expression on the diversity of immunoglobulin CDR3 regions and the subsequent effects on fetal perinatal and adult B cells will be determined. This question will be addressed by the use of transgenic mice in which N region additions will be introduced during stages of B cell development when such additions are normally absent or minimal. The molecular and cellular differences between B cell subsets will be compared by study of precursor/progeny relationships using newly developed monoclonal antibodies as cellular markers and the use of transgenic mice in which B cells constitutively express CD5. The overall goal of these studies is to understand the differentiative events during early development that mold the B cell repertoire. It will be determined whether a restricted perinatal B cell repertoire is more important to the development of a healthy immune system than a highly diverse adult B cell repertoire. The experiments outlined in this proposal will aid in our understanding of the role that these fetal and neonatal B cells play in establishment and maintenance of the normal immune system and will provide insight into their roles in autoimmune diseases, B cell neoplasia and immunodeficiency diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI014782-20
Application #
2671693
Study Section
Immunobiology Study Section (IMB)
Project Start
1978-09-01
Project End
2000-03-31
Budget Start
1998-04-01
Budget End
1999-03-31
Support Year
20
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
University of Alabama Birmingham
Department
Microbiology/Immun/Virology
Type
Schools of Dentistry
DUNS #
004514360
City
Birmingham
State
AL
Country
United States
Zip Code
35294

  Publications

Wang, Yong; Schafer, Cara C; Hough, Kenneth P et al. (2018) Myeloid-Derived Suppressor Cells Impair B Cell Responses in Lung Cancer through IL-7 and STAT5. J Immunol 201:278-295
Dickinson, Gregory S; Levenson, Eric A; Walker, Justin A et al. (2018) IL-7 Enables Antibody Responses to Bacterial Polysaccharides by Promoting B Cell Receptor Diversity. J Immunol 201:1229-1240
Patel, Preeyam S; Kearney, John F (2017) CD36 and Platelet-Activating Factor Receptor Promote House Dust Mite Allergy Development. J Immunol 199:1184-1195
Hammad, Hamida; Vanderkerken, Matthias; Pouliot, Philippe et al. (2017) Transitional B cells commit to marginal zone B cell fate by Taok3-mediated surface expression of ADAM10. Nat Immunol 18:313-320
Azzam, Kathleen M; Madenspacher, Jennifer H; Cain, Derek W et al. (2017) Irgm1 coordinately regulates autoimmunity and host defense at select mucosal surfaces. JCI Insight 2:
Patel, Preeyam S; King, R Glenn; Kearney, John F (2016) Pulmonary ?-1,3-Glucan-Specific IgA-Secreting B Cells Suppress the Development of Cockroach Allergy. J Immunol 197:3175-3187
New, J Stewart; King, R Glenn; Kearney, John F (2016) Manipulation of the glycan-specific natural antibody repertoire for immunotherapy. Immunol Rev 270:32-50
Patel, Preeyam; Kearney, John F (2016) Immunological Outcomes of Antibody Binding to Glycans Shared between Microorganisms and Mammals. J Immunol 197:4201-4209
Kearney, John F; Patel, Preeyam; Stefanov, Emily K et al. (2015) Natural antibody repertoires: development and functional role in inhibiting allergic airway disease. Annu Rev Immunol 33:475-504
Wharton, Rebekah E; Stefanov, Emily K; King, R Glenn et al. (2015) Antibodies generated against Streptococci protect in a mouse model of disseminated aspergillosis. J Immunol 194:4387-96

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