Abstract

Interferons (IFNs), a family of cytokines with diverse biological functions, including anti-tumor and immunomodulatory actions, are a crucial component of a network of regulatory substances which maintain homeostasis for multicellular organisms. The overall goal of the Program Project is to develop a comprehensive account of signaling in the IFN system from receptors to genes. IFNs bind specific cell surface receptors, eliciting signals which culminate in transcriptional activation of a set of genes, termed IFN-stimulated genes (ISG), which encode proteins believed to be the biological effectors of IFN treatment. The current level of understanding of IFN(alpha) has been achieved by the application of biochemistry, genetics, and molecular biology, to which our group has made substantial contributions. The Program Project is composed of six research projects, a Tissue Culture Core, and a centralized Administrative Core. The individual proposals are highly focused but are well integrated into an overall research plan. We propose to use genetic experimental approaches to complement traditional biochemical and molecular biologic methods to isolate and characterize the components of signaling pathways, as reflected in the research proposals of the individual investigators and by the overall plan of the Program Project. Project 1 is directly focused on the genetic approach to signaling, including the generation of mutant cell lines selectively deficient for IFN signaling and development of techniques for rapidly complementing these mutants. Signaling components will be functionally analyzed, partially through the use of defective cell lines and extracts prepared from such cells. In Project 2, these techniques will be extended to address ISGF3-independent signaling pathways. Project 3 addresses signaling crosstalk between IFN(gamma) and TGFBetaI. Project 4 proposes a strategy for abrogating expression of specific genes, using an antisense-targeted, IFN-inducible endoribonuclease strategy. This approach will have obvious applicability for selected experiment in other projects. Project 5 is directed at the mechanisms through which dsRNA can induce both IFN sensitive and insensitive genes. Project 6 is focused upon the role of Rel homology genes and kappa(B) sequence motifs in mediating response to IFN(gamma) and LPS. The components of this Program Project are complementary, by virtue of their relation to the major themes of the program, their interactive nature, and, administratively, by their use of the common facilities house in the Cores.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA062220-02
Application #
2103320
Study Section
Special Emphasis Panel (SRC (28))
Project Start
1994-08-15
Project End
1999-05-31
Budget Start
1995-06-01
Budget End
1996-05-31
Support Year
2
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Cleveland Clinic Lerner
Department
Type
DUNS #
017730458
City
Cleveland
State
OH
Country
United States
Zip Code
44195

  Publications

Sarvestani, Samaneh K; Signs, Steven A; Lefebvre, Veronique et al. (2018) Cancer-predicting transcriptomic and epigenetic signatures revealed for ulcerative colitis in patient-derived epithelial organoids. Oncotarget 9:28717-28730
Cai, Gang; Zhu, Liang; Chen, Xing et al. (2018) TRAF4 binds to the juxtamembrane region of EGFR directly and promotes kinase activation. Proc Natl Acad Sci U S A 115:11531-11536
Herjan, Tomasz; Hong, Lingzi; Bubenik, Jodi et al. (2018) IL-17-receptor-associated adaptor Act1 directly stabilizes mRNAs to mediate IL-17 inflammatory signaling. Nat Immunol 19:354-365
Veleeparambil, Manoj; Poddar, Darshana; Abdulkhalek, Samar et al. (2018) Constitutively Bound EGFR-Mediated Tyrosine Phosphorylation of TLR9 Is Required for Its Ability To Signal. J Immunol 200:2809-2818
Nan, Jing; Wang, Yuxin; Yang, Jinbo et al. (2018) IRF9 and unphosphorylated STAT2 cooperate with NF-?B to drive IL6 expression. Proc Natl Acad Sci U S A 115:3906-3911
Zhou, Hao; Bulek, Katarzyna; Li, Xiao et al. (2017) IRAK2 directs stimulus-dependent nuclear export of inflammatory mRNAs. Elife 6:
Wang, Chenhui; Zhang, Cun-Jin; Martin, Bradley N et al. (2017) IL-17 induced NOTCH1 activation in oligodendrocyte progenitor cells enhances proliferation and inflammatory gene expression. Nat Commun 8:15508
Wang, Yuxin; Nan, Jing; Willard, Belinda et al. (2017) Negative regulation of type I IFN signaling by phosphorylation of STAT2 on T387. EMBO J 36:202-212
Doherty, Mary R; Cheon, HyeonJoo; Junk, Damian J et al. (2017) Interferon-beta represses cancer stem cell properties in triple-negative breast cancer. Proc Natl Acad Sci U S A 114:13792-13797
Liu, Caini; Zhu, Liang; Fukuda, Koichi et al. (2017) The flavonoid cyanidin blocks binding of the cytokine interleukin-17A to the IL-17RA subunit to alleviate inflammation in vivo. Sci Signal 10:

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