Abstract

The overall focus of the proposed research is to define, at the level of chromatin regulation, the molecular processes underlying expression of the IL-4, IL-5 and IL-13 genes in T cells and other cell types. These three genes are closely linked on mouse chromosome 11 and human chromosome 5. They are expressed by T helper type 2 (Th2) cells, mast cells, and certain other cell types; they are silenced in T helper type 1 (Thl) cells as well as most non-lymphoid cells. Within the conserved cytokine cluster, the IL-13 and IL-5 genes are separated by the RAD50 gene, which encodes an essential DNA repair protein that is expressed by all cells. During the last project period, DNase I hypersensitivity mapping and comparative genome sequence analyses revealed (with striking correspondence) a large number of potential regulatory regions in the IL-4/IL-13/RAD50/IL-5 locus. Deletion of three of these regions, CNS-1, DH sites V/VA and DH site IV, in the genomic context has confirmed their regulatory function; DH site IV is the first negative (silencer) element to be defined in the locus. The objective for this competing renewal application is to build on these data to understand gene regulation of the IL-4/ IL-13/ RAD50/ IL-5 locus at a more mechanistic level. Using a combination of biochemical and gene-targeting approaches, the early and late events which lead to activation or silencing at this locus will be delineated and the functional roles of selected transcription factors and regulatory elements will be explored. Specific objectives are to define the role of the known or presumed elements DH site IV andHSS3 (Aim 1); to define the role of the positive elements CNS-1 and CNS-2 (Aim 2); to explore the function of potential regulatory elements in the RAD50 gene (Aim 3); and to investigate the role of GATA3 (Aim 4). These experiments will elucidate the molecular basis for coordinate expression and silencing of the cytokine genes, and should provide clues to the mechanisms underlying irreversible lineage commitment to the Th2 or Th1 phenotype. The question is important given the striking pathologies associated with progressive Th1/Th2 polarisation in response to chronic antigen stimulation in vivo: chronic Th2 responses are associated with asthma and atopy, while Th1 cells are implicated in inflammation and autoimmune disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI044432-10
Application #
7473230
Study Section
Immunobiology Study Section (IMB)
Program Officer
Dong, Gang
Project Start
1999-07-01
Project End
2009-11-30
Budget Start
2008-07-01
Budget End
2009-11-30
Support Year
10
Fiscal Year
2008
Total Cost
$545,883
Indirect Cost

  Institution

Name
Immune Disease Institute, Inc.
Department
Type
DUNS #
059709394
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Tsagaratou, Ageliki; González-Avalos, Edahí; Rautio, Sini et al. (2017) TET proteins regulate the lineage specification and TCR-mediated expansion of iNKT cells. Nat Immunol 18:45-53
Lio, Chan-Wang; Zhang, Jiayuan; González-Avalos, Edahí et al. (2016) Tet2 and Tet3 cooperate with B-lineage transcription factors to regulate DNA modification and chromatin accessibility. Elife 5:
Äijö, Tarmo; Huang, Yun; Mannerström, Henrik et al. (2016) A probabilistic generative model for quantification of DNA modifications enables analysis of demethylation pathways. Genome Biol 17:49
Äijö, Tarmo; Yue, Xiaojing; Rao, Anjana et al. (2016) LuxGLM: a probabilistic covariate model for quantification of DNA methylation modifications with complex experimental designs. Bioinformatics 32:i511-i519
Yue, Xiaojing; Trifari, Sara; Äijö, Tarmo et al. (2016) Control of Foxp3 stability through modulation of TET activity. J Exp Med 213:377-97
An, Jungeun; González-Avalos, Edahí; Chawla, Ashu et al. (2015) Acute loss of TET function results in aggressive myeloid cancer in mice. Nat Commun 6:10071
Balasubramani, Anand; Larjo, Antti; Bassein, Jed A et al. (2015) Cancer-associated ASXL1 mutations may act as gain-of-function mutations of the ASXL1-BAP1 complex. Nat Commun 6:7307
Ko, Myunggon; An, Jungeun; Pastor, William A et al. (2015) TET proteins and 5-methylcytosine oxidation in hematological cancers. Immunol Rev 263:6-21
Ko, Myunggon; An, Jungeun; Rao, Anjana (2015) DNA methylation and hydroxymethylation in hematologic differentiation and transformation. Curr Opin Cell Biol 37:91-101
Kang, Jinsuk; Lienhard, Matthias; Pastor, William A et al. (2015) Simultaneous deletion of the methylcytosine oxidases Tet1 and Tet3 increases transcriptome variability in early embryogenesis. Proc Natl Acad Sci U S A 112:E4236-45

Showing the most recent 10 out of 67 publications