Abstract

Rejection remains a major hurdle to long lasting transplant survival and we aspire to uncover the fundamental mechanisms that hinder stable allograft survival. In the last funding period, we studied the mechanisms of Treg dysfunctions and identified BATF and BATF3 as potent repressors of Foxp3, suppressing Foxp3 expression and Treg induction. These studies also led to the discovery of the DHX15 helicase as a critical regulator of Foxp3+Tregs, as conditional deletion of Dhx15 in Tregs resulted in a profound depletion of Tregs in the periphery and lethal autoimmune diseases. In essence, DHX15 is an RNA helicase (an RNA binding motor protein) and traditionally thought to be involved in RNA processing. Its roles in the control of Tregs are unexpected and clearly reveal novel previously unknown aspects of Tregs that are different from currently known mechanisms, and uncovering those mechanisms is the central goal of this proposal. Our working hypothesis is that DHX15 controls Treg identity and/or survival at peripheral sites and that its deficiency results in either their reversion to Teff or die of apoptosis. We surmise that DHX15 may also control Tregs at the graft site, where they must overcome the inflammatory milieu to exert suppressive functions. We proposed 3 Aims to test this hypothesis in this application:
the first Aim i s to test whether DHX15 controls Treg identity by acting as an RNA splicing factor, processing mRNAs that encode the Foxp3 or Foxp3 controlled signature molecules in Tregs, the second Aim is to address whether DHX15 controls Tregs survival by regulating the IL-2 signaling complex, such that Tregs die of apoptosis in its absence, and the third Aim is to examine whether DHX15 is especially important for Tregs at graft sites where they are needed the most in promoting transplant tolerance. Overall, DHX15 is the first RNA helicase identified thus far that controls Tregs, and the genetically modified models as well as cutting-edge approaches we have developed put us in a unique position in dissecting mechanistically how the DHX15 helicase acts in regulating Tregs, an area of considerable importance in both basic Treg biology and Treg- based therapies.

Public Health Relevance

The potential of organ transplantation as a lifesaving therapy is limited by the immunosuppression drug- induced toxicities and progressive loss of organ transplants. Our project is designed to uncover the new and fundamental barriers that hinder transplant survival. Our proposed studies will open new opportunities in the development of better therapies for transplant patients, as well as for patients with autoimmune diseases, bone marrow grafts, and cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
2R01AI106200-06
Application #
10217440
Study Section
Transplantation, Tolerance, and Tumor Immunology Study Section (TTT)
Program Officer
Kehn, Patricia J
Project Start
2014-02-01
Project End
2026-01-31
Budget Start
2021-02-01
Budget End
2022-01-31
Support Year
6
Fiscal Year
2021
Total Cost
Indirect Cost

  Institution

Name
Methodist Hospital Research Institute
Department
Type
DUNS #
185641052
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Zhang, Xiaolong; Xiao, Xiang; Lan, Peixiang et al. (2018) OX40 Costimulation Inhibits Foxp3 Expression and Treg Induction via BATF3-Dependent and Independent Mechanisms. Cell Rep 24:607-618
Xiao, Xiang; Fan, Yihui; Li, Junhui et al. (2018) Guidance of super-enhancers in regulation of IL-9 induction and airway inflammation. J Exp Med 215:559-574
Lan, Peixiang; Fan, Yihui; Zhao, Yue et al. (2017) TNF superfamily receptor OX40 triggers invariant NKT cell pyroptosis and liver injury. J Clin Invest 127:2222-2234
Fischer, Julius Clemens; Otten, Vera; Kober, Maike et al. (2017) A20 Restrains Thymic Regulatory T Cell Development. J Immunol 199:2356-2365
Li, Junhui; Chen, Shuqiu; Xiao, Xiang et al. (2017) IL-9 and Th9 cells in health and diseases-From tolerance to immunopathology. Cytokine Growth Factor Rev 37:47-55
Wu, Jie; Zhang, Hedong; Shi, Xiaomin et al. (2017) Ablation of Transcription Factor IRF4 Promotes Transplant Acceptance by Driving Allogenic CD4+ T Cell Dysfunction. Immunity 47:1114-1128.e6
Xiao, Xiang; Shi, Xiaomin; Fan, Yihui et al. (2016) The Costimulatory Receptor OX40 Inhibits Interleukin-17 Expression through Activation of Repressive Chromatin Remodeling Pathways. Immunity 44:1271-83
Xiao, Xiang; Shi, Xiaomin; Fan, Yihui et al. (2015) GITR subverts Foxp3(+) Tregs to boost Th9 immunity through regulation of histone acetylation. Nat Commun 6:8266
Chen, Wenhao; Ghobrial, Rafik M; Li, Xian C (2015) The Evolving Roles of Memory Immune Cells in Transplantation. Transplantation 99:2029-37