The aim of this project is to understand how Fc receptors communicate intracellular signals to initiate mast cell activation leading to inflammation. Fc receptors are key players in autoimmune diseases like systemic lupus erythematosus and in allergic disease. We have focused on signaling proteins that may serve as possible links from Fc receptor to gene expression and mast cell degranulation and on how this receptors activity is regulated. This focus is based on increaing the knowledge of potential therapeutic targets in autoimmune and allergic disease. ? ? Results: The objectives of the past year were met in the following manner. First, Studies on the role of two different isoforms of Lyn kinase that associate with the IgE receptor were initiated. These studies led us to explore the influence of genetics on the role of these kinases and their ability to activate mast cells. We found that differences in the genetic background of mice has a dramatic effect both on the function of these kinases and their control on mast cell responses. Second, additional work explored whether other stimuli that lead to mast cell activation functioned through the use of Lyn or Fyn. Third, we also have initial findings suggesting that Fyn kinase interacts with the beta subunit of the IgE receptor and that it may compete with Lyn for this binding. This suggest the existence of receptor heterogeniety, some associated with Fyn whereas others with Lyn. Fourth: Addtionally, the work of this year also led to the discovery that their is differential dephosphorylation of the two tyrosine resdiues found in the cytoplasmic domain of the gamma subunit of the IgE receptor and that this is important as a inactivation step that controls the extent of mast cell activation by controlling the activation of Syk kinase, a kinase that amplifies IgE receptor signalling. ? ? Conclusions and Significance: In summary, we found that both Fyn and Lyn kinases function is regulated in the context of other genes, as it was found that mice with differing genetic backgrounds had different kinase levels and mast cell responses were influenced by the levels of the kinases being expressed. These findings provide new avenues for future exploration toewards understanding the role of IgE Fc receptors in health and disease.

Project Start
Project End
Budget Start
Budget End
Support Year
15
Fiscal Year
2008
Total Cost
$1,419,961
Indirect Cost
Name
National Institute of Arthritis and Musculoskeletal and Skin Diseases
Department
Type
DUNS #
City
State
Country
United States
Zip Code
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