Abstract

It is now well established that the onset of T cell development is initiated by the induction of Notch expression. During the previous grant cycle, we found that this critical step is controlled by the combined activities of E2A and HEB. Once Notch1 expression is activated, Notch signaling acts in concert with RUNX1, TCF1, E2A and GATA-3 to activate Bcl11b expression. Bcl11b next acts in concert with E2A to activate a T-lineage specific gene program. We (with Project 1) also demonstrated that E2A activates the expression of a non-coding transcript, named ThymoD, to reposition the Bcl11b enhancer from the nuclear lamina to the nuclear interior. These studies linked E-protein occupancy, non-coding transcription and Bcl11b expression into a common pathway that orchestrates the ?? versus ?? T cell fate decision. We now aim to describe, in physical and kinetic terms, Bcl11b locus movement relative to the onset of T cell development. To track genomic interactions in live lymphoid cells, we have developed a novel strategy. Specifically, we tracked the motion of DNA elements to visualize VDJ recombination in live B cells using tandem arrays of WT-TET and MUT-TET repressor binding sites. We propose to use the same strategy to describe in live T cells the trajectories of Bcl11b enhancer- promoter communication. Specifically, we will examine how Bcl11b enhancer-promoter communication is suppressed when sequestered at the nuclear lamina prior to commitment to the T cell lineage and after these loci return to the lamina upon adoption of the ?? T cell fate (with Projects 1 and 3). We will also examine how E-proteins and Notch signaling modulate Bcl11b enhancer-promoter communication to establish and maintain ?? T cell identity (with Projects 2 and 3) and how E-proteins, Notch signaling, non-coding transcription and nuclear repositioning are linked in four-dimensional space to orchestrate ?? T cell fate. Collectively these studies proposed here would be a first step towards describing the ?? versus ?? T cell fate choice in four- dimensional space and would not be possible outside of this integrated programmatic effort.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI102853-07
Application #
9989065
Study Section
Special Emphasis Panel (ZAI1)
Project Start
2014-05-15
Project End
2024-07-31
Budget Start
2020-08-01
Budget End
2021-07-31
Support Year
7
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
Research Institute of Fox Chase Cancer Center
Department
Type
DUNS #
064367329
City
Philadelphia
State
PA
Country
United States
Zip Code
19111

  Publications

Fahl, Shawn P; Coffey, Francis; Kain, Lisa et al. (2018) Role of a selecting ligand in shaping the murine ??-TCR repertoire. Proc Natl Acad Sci U S A 115:1889-1894
Zarin, Payam; In, Tracy Sh; Chen, Edward Ly et al. (2018) Integration of T-cell receptor, Notch and cytokine signals programs mouse ?? T-cell effector differentiation. Immunol Cell Biol 96:994-1007
Zhang, Baojun; Jiao, Anjun; Dai, Meifang et al. (2018) Id3 Restricts ?? NKT Cell Expansion by Controlling Egr2 and c-Myc Activity. J Immunol 201:1452-1459
Murre, Cornelis (2018) 'Big bang' of B-cell development revealed. Genes Dev 32:93-95
Roy, Sumedha; Moore, Amanda J; Love, Cassandra et al. (2018) Id Proteins Suppress E2A-Driven Invariant Natural Killer T Cell Development prior to TCR Selection. Front Immunol 9:42
Chisolm, Danielle A; Savic, Daniel; Moore, Amanda J et al. (2017) CCCTC-Binding Factor Translates Interleukin 2- and ?-Ketoglutarate-Sensitive Metabolic Changes in T Cells into Context-Dependent Gene Programs. Immunity 47:251-267.e7
Li, Jia; Roy, Sumedha; Kim, Young-Mi et al. (2017) Id2 Collaborates with Id3 To Suppress Invariant NKT and Innate-like Tumors. J Immunol 198:3136-3148
Zhu, Yina; Gong, Ke; Denholtz, Matthew et al. (2017) Comprehensive characterization of neutrophil genome topology. Genes Dev 31:141-153
Miyazaki, Masaki; Miyazaki, Kazuko; Chen, Kenian et al. (2017) The E-Id Protein Axis Specifies Adaptive Lymphoid Cell Identity and Suppresses Thymic Innate Lymphoid Cell Development. Immunity 46:818-834.e4
Moore, Amanda J; In, Tracy Sh; Trotman-Grant, Ashton et al. (2017) A key role for IL-7R in the generation of microenvironments required for thymic dendritic cells. Immunol Cell Biol 95:933-942

Showing the most recent 10 out of 23 publications