Abstract

All hematopoietic cell types arise from pluripotent stem cells through multiple steps of lineage commitment and subsequent maturation. Cellular decisions regarding proliferation and differentiation are tightly controlled to ensure homeostasis of all circulating blood cells. Disruption of this control can lead to hematological aplasias or malignancies. The efforts of this laboratory are directed towards understanding the development of the erythroid cell lineage by focusing on the transcription factor GATA-1. GATA-1 participates in the regulation of virtually all erythroid-restricted genes including the globin genes. It causes cell cycle arrest and prevents apoptosis of erythroid precursor cells. This project centers around our recent observation that the transcriptional integrator CBP serves as cofactor for GATA-1 and is required for erythroid cell maturation. In addition to GATA-1, CBP regulates various transcription factors involved in cellular differentiation and is associated with translocations found in certain types of leukemias. CBP possesses histone acetylase activity towards all four core histones. Recently, we have discovered that CBP acetylates GATA-1 specifically at functionally important sites.
Under Aim 1 we will determine the precise residues of GATA-1 acetylated in vitro and in vivo. Subsequently, we will monitor acetylation of GATA-1 in vivo during cell cycle progression and cellular differentiation.
In Aim 2 we will analyze the functional consequences of GATA-1 acetylation through biochemical assays and through gene complementation experiments using a unique GATA-1-deficient erythroid cell line. This cell line allows the testing of GATA-1 constructs in the physiological environment of maturing erythroid cells. Studies outlined in Aim 3 are designed to delineate the transcriptional pathways by which CBP controls erythroid maturation. Using various cellular assays, we will determine which domains of CBP are required for erythroid differentiation and GATA-1 activation. Together, these studies should provide new insights into the mechanisms by which cellular differentiation and tissue-specific gene expression is accomplished and might lead to novel approaches for therapy of hematopoietic disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
1R01DK054937-01
Application #
2740973
Study Section
Hematology Subcommittee 2 (HEM)
Program Officer
Badman, David G
Project Start
1999-03-01
Project End
2003-02-28
Budget Start
1999-03-01
Budget End
2000-02-29
Support Year
1
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Children's Hospital of Philadelphia
Department
Type
DUNS #
073757627
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Philipsen, Sjaak; Hardison, Ross C (2018) Evolution of hemoglobin loci and their regulatory elements. Blood Cells Mol Dis 70:2-12
Bartman, Caroline R; Hamagami, Nicole; Keller, Cheryl A et al. (2018) Transcriptional Burst Initiation and Polymerase Pause Release Are Key Control Points of Transcriptional Regulation. Mol Cell :
Behera, Vivek; Evans, Perry; Face, Carolyne J et al. (2018) Exploiting genetic variation to uncover rules of transcription factor binding and chromatin accessibility. Nat Commun 9:782
Wai, Dorothy C C; Szyszka, Taylor N; Campbell, Amy E et al. (2018) The BRD3 ET domain recognizes a short peptide motif through a mechanism that is conserved across chromatin remodelers and transcriptional regulators. J Biol Chem 293:7160-7175
Grevet, Jeremy D; Lan, Xianjiang; Hamagami, Nicole et al. (2018) Domain-focused CRISPR screen identifies HRI as a fetal hemoglobin regulator in human erythroid cells. Science 361:285-290
Hsu, Sarah C; Gilgenast, Thomas G; Bartman, Caroline R et al. (2017) The BET Protein BRD2 Cooperates with CTCF to Enforce Transcriptional and Architectural Boundaries. Mol Cell 66:102-116.e7
Hsiung, Chris C-S; Blobel, Gerd A (2016) A new bookmark of the mitotic genome in embryonic stem cells. Nat Cell Biol 18:1124-1125
Edwards, Christopher R; Ritchie, William; Wong, Justin J-L et al. (2016) A dynamic intron retention program in the mammalian megakaryocyte and erythrocyte lineages. Blood :
Stonestrom, Aaron J; Hsu, Sarah C; Werner, Michael T et al. (2016) Erythropoiesis provides a BRD's eye view of BET protein function. Drug Discov Today Technol 19:23-28
Stonestrom, Aaron J; Hsu, Sarah C; Jahn, Kristen S et al. (2015) Functions of BET proteins in erythroid gene expression. Blood 125:2825-34

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