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Vermont Cobre: Project 2: Innate Immune Responses to Cryptosporidium Parvum

Investigators
Kirkpatrick, Beth Diane
Institutions
University of Vermont
Start date
2006
End date
2007
Objective
Cryptosporidium parvum is an important global cause of persistent and chronic diarrhesa. In young children, particularly in underdeveloped countries, cryptosporidiosis is clinically more severe and is associated with more intestinal inflammation than infection in adults. Little is understood about the mucosal 'innate' immune respone to C. parvum. Gamma delta (y6) T cells are an important T cell population in young children and in the intestinal tract. In response to infection at the intestine, T cells appear to expand in the periphery and selectively 'home' back to the intestinal mucosa, via gut-specific homing receptors (a4p7, aEp7). Intestinal yd T cells appear to modulate recovery of the epithelium, respond to intestinal 'stress' and may have important cytolytic function, especially in killing of infected intestinal epithelial cells (and possibly CD4+ ap T cells).

This proposal seeks to train the investigator in classic and molecular/genetic immunology techniques and to apply this basic science knowledge to study mucosal immune responses to cryptosporidiosis in children, especially those in the developing world. The proposal hypotheses that o T cells are important in the innate immune response to cryptosporidiosis, are activated in response to C. parvum via the T cell receptor with necessary co-stimulation by the gut-specific MHC-I molecule (MIC-A), and kill infected epithelial cells by cytolysis and apoptosis.

This information will then be applied to the study of gamma delta T cells from a small population of Bangladeshi children with acute cryptosporidiosis to demonstrate in vivo relevance. The primary mentor of this proposal is a full professor of Immunology with expertise in y6 T cells and with a laboratory skilled in the proposed research assays

In the research proposal, Aim 1 establishes whether the activation of the y5 cells is via the TCR and requires co-stimulation with the MHC-I like molecule MIC-A. In this aim, cloned y and y chains of the T cell receptor are transfected to a T cell receptor negative cell line and evaluated for function.

Aim 2 evaluates the cytotoxicity of y5 via Fas-FasL and perforin and confirms whether cytotoxicity is antigen-dependent.

Finally, to establish in vivo relevance, Aim 3 examines the y5 T cells from children with cryptosporidiosis, establishes whether these y6 cells (carrying gut homing receptors) can be extracted from peripheral lymphocytes and if these clones have activation and cytolytic functions similar to the in vitro data.

These data will advance our understanding of the mucosal immune response to cryptosporidiosis, which will lead to further advances in prevention and th

Funding Source
Nat'l. Center for Research Resources
Project number
1P20RR021905-01
Categories
Cryptosporidium