Abstract

The transcription factor NF-icB plays a criticalrole in innate immune responses by augmenting the expression of many inducible, immediate response genes, including IL-1,IL-2, IL-2Ra, IL-6, IL-8,1L-12,TNF-a, p-IFN, GM-CS r, COX-2, E-selectin and serum amyloid A protein. NF-KB acts as a critical co-ordinating element in the body's response to infection and injury, and thus is an important mediator of innate immunity. Recent studies demonstrating the importance of NF-KB activation by signaling through the Toll-receptors has highlighted their evolutionarilyconserved role in host response to pathogens. It is also an essential element for the replication of different viruses, including HIV. NF-KB also serves as an important anti-apoptotic factor in many biological systems and its aberrant activation has been linked to the development of certain forms of cancer. Therefore understanding how NF-KB activity is regulated has great relevance for the development of novel therapies for the treatment of inflammatory diseases and cancer. The primary long-term objective of our research is to determine how the signals from the Toll-receptors, that induce the activity of NF-KB, are transduced and lead to the mounting of innate immune responses. In this application we propose to study the Toll-receptor signal transduction pathway by focusing on two novel adapter proteins, ECSIT and X, that we have recently isolated. We will use a variety of approaches, including generation and analysis of gene targeted animals, to study these molecules. We will also try to isolate potential adapter proteins that bind to the Toll- receptors and substitute for MyD88. We wish to delineate the sequence of events that are responsible for the induction of the 1KBkinase (IKK) complex activity in response to signalingfrom Toll-receptors. In particular we wish to understand the role of NEMO/IKKy, the regulatory subunit of the IKK complex in the activation process, Finally we will study the possible mechanisms by which the IKK proteins facilitate the proteosomal degradation of phosphorylated and ubiquitinated 1KB substrates. PERFORMANCE S1TE(S) (organization, city, state) Yale University School of Medicine New Haven. CT 06510 KEY PERSONNEL. See instructions on Page 11. Usecontinuationpages as neededto provide the required information in the format shown below. Name Organization Role on Project Sankar Ghosh Yale Medical School Principal Investigator Michael J. May Yale Medical School Associate Research Scientist Richard A. Flavell Yale Medical School Collaborator/consultant Brigid Hogan Vanderbilt University Collaborator/consultant PHS 398 I Rev. 4/98) Page 2 B B Number p;,ges consecutively at the bottom throughout the application. Do not use suffixes such as 3a, 3b. CC Principa^fcstigator/Program Director (Last, first, middle): Type the name of the principal investigator/prograPtlirector at the top of eachprintedpage and each continu^Pi page. (For type specifications, see instructions on page 6.) RESEARCHGRANT TABLE OF CONTENTS Page Numbers Face Page 1 Description,

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37AI033443-15
Application #
7232389
Study Section
Special Emphasis Panel (NSS)
Program Officer
Palker, Thomas J
Project Start
1993-09-01
Project End
2011-05-31
Budget Start
2007-06-01
Budget End
2008-05-31
Support Year
15
Fiscal Year
2007
Total Cost
$400,538
Indirect Cost

  Institution

Name
Yale University
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
043207562
City
New Haven
State
CT
Country
United States
Zip Code
06520

  Publications

Grinberg-Bleyer, Yenkel; Caron, Rachel; Seeley, John J et al. (2018) The Alternative NF-?B Pathway in Regulatory T Cell Homeostasis and Suppressive Function. J Immunol 200:2362-2371
Seeley, John J; Baker, Rebecca G; Mohamed, Ghait et al. (2018) Induction of innate immune memory via microRNA targeting of chromatin remodelling factors. Nature 559:114-119
Grinberg-Bleyer, Yenkel; Oh, Hyunju; Desrichard, Alexis et al. (2017) NF-?B c-Rel Is Crucial for the Regulatory T Cell Immune Checkpoint in Cancer. Cell 170:1096-1108.e13
Oh, Hyunju; Grinberg-Bleyer, Yenkel; Liao, Will et al. (2017) An NF-?B Transcription-Factor-Dependent Lineage-Specific Transcriptional Program Promotes Regulatory T Cell Identity and Function. Immunity 47:450-465.e5
Hatai, Hirotsugu; Lepelley, Alice; Zeng, Wangyong et al. (2016) Toll-Like Receptor 11 (TLR11) Interacts with Flagellin and Profilin through Disparate Mechanisms. PLoS One 11:e0148987
Dainichi, Teruki; Hayden, Matthew S; Park, Sung-Gyoo et al. (2016) PDK1 Is a Regulator of Epidermal Differentiation that Activates and Organizes Asymmetric Cell Division. Cell Rep 15:1615-23
Castellanos-Rubio, Ainara; Fernandez-Jimenez, Nora; Kratchmarov, Radomir et al. (2016) A long noncoding RNA associated with susceptibility to celiac disease. Science 352:91-5
Postler, Thomas S; Ghosh, Sankar (2015) Bridging the Gap: A Regulator of NF-?B Linking Inflammation and Cancer. J Oral Biosci 57:143-147
Yu, Minjun; Owens, David M; Ghosh, Sankar et al. (2015) Conditional PDK1 Ablation Promotes Epidermal and T-Cell-Mediated Dysfunctions Leading to Inflammatory Skin Disease. J Invest Dermatol 135:2688-2696
Grinberg-Bleyer, Yenkel; Dainichi, Teruki; Oh, Hyunju et al. (2015) Cutting edge: NF-?B p65 and c-Rel control epidermal development and immune homeostasis in the skin. J Immunol 194:2472-6

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