Host innate immune-microbial interactions and intestinal inflammation
Project Number1P01DK094779-01A1
Contact PI/Project LeaderSARTOR, RYAN B
Awardee OrganizationUNIV OF NORTH CAROLINA CHAPEL HILL
Description
Abstract Text
DESCRIPTION (provided by applicant): Interactions between the host innate immune system and the enteric microbiota are proximal events in the pathogenesis of the idiopathic human inflammatory bowel diseases (IBD). Solving the pathogenesis of IBD and ultimately curing and preventing these chronic, debilitating conditions depends on using experimental models and human systems to better understand functional interactions between innate immunity and enteric microbes that determine differentiation and activation of effector vs. regulatory T cell subsets in mucosal tissues. We hypothesize that subsets of the commensal microbiota preferentially activate protective vs. destructive innate signaling pathways that integratively activate mucosal innate and antigen presenting cells to secrete cytokines that promote regulatory vs. effector T cell responses. These interacting bacterially- activated innate and adaptive pathways mediate homeostatic vs. effector immune responses and can be manipulated for therapeutic purposes. This hypothesis will be addressed through synergistic efforts of six fully integrated investigators with complementary expertise in innate immunity and host-microbiota interactions, facilitated by two highly utilized cores. Project 1 (Jenny Ting): "NOD-like receptors in intestinal inflammation". Project 2 (Balfour Sartor): "Role of IL-10 in APC regulation of protective vs. pathogenic T cell responses to commensal bacteria". Project 3 (Scott Plevy): "Macrophage IL-10 and IL-12 regulation by the enteric microbiota in intestinal inflammation ". Project 4 (John Rawls): "Microbial regulation of systemic neutrophil function". The Project Leaders will be supported by two highly interactive cores that have already facilitated collaborative research. Core A: Gnotobiotic and Transgenic Rodent and Zebrafish Core (Core Co- Directors, Drs. Sartor and Rawls). Core B: Human Tissue and Genomics Core (Co-Directors, Drs. Scott Plevy, Hans Herfarth and Shehzad Sheikh). The investigators, facilitated by Cores, are poised to accelerate the understanding of how the innate immune system interacts with the enteric microbiota in health and disease. This knowledge could have a major public health impact upon IBD and the numerous disorders that result from dysregulated innate immune interactions with enteric microbiota.
National Institute of Diabetes and Digestive and Kidney Diseases
CFDA Code
847
DUNS Number
608195277
UEI
D3LHU66KBLD5
Project Start Date
19-September-2013
Project End Date
30-June-2018
Budget Start Date
19-September-2013
Budget End Date
30-June-2014
Project Funding Information for 2013
Total Funding
$1,528,537
Direct Costs
$1,133,701
Indirect Costs
$394,836
Year
Funding IC
FY Total Cost by IC
2013
National Institute of Diabetes and Digestive and Kidney Diseases
$1,528,537
Year
Funding IC
FY Total Cost by IC
Sub Projects
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