Abstract

Our goal is to understand the molecular mechanisms that regulate the emergence and subsequent transitions of the hemato-vascular program during development. This should facilitate progress toward manipulating stem and progenitor cell populations, modulating differentiation of specific lineages, and impacting treatment strategies for certain leukemias. We identified the BMP signaling pathway as essential for the generation of the initial hematopoietic system, and we characterized the function of several interacting pathways. In the last funding cycle we discovered that Smad signaling promotes expansion of the earliest hemato-vascular progenitors (the hemangioblast), yet also restricts the proliferation of these cells in order to maintain a stem cell population and control the development of committed progenitors. Our results indicate that Smad-dependent pathways continue to regulate hematopoiesis in the definitive lineage and even in the adult. Due to compensation and/or embryonic lethality it is challenging to study in vivo the role of BMP signaling components. This renewal application proposes to investigate lineage and stage-specific functions for Smad signaling during hematopoietic developmental transitions, to understand the specificity of function among Smads, and to define molecular mechanisms by which Smad activity regulates the commitment of stem and progenitor cells to hemato-vascular fates. The proposal exploits complementary experimental advantages of the zebrafish model and murine ES cells to understand how stem and progenitor cell populations are normally regulated by conserved Smad-dependent molecular pathways, considering that these might ultimately be modulated for clinical benefit.
The Aims are to: 1. Define the spatio-temporal requirements of Smad signaling for hemato-vascular development. We will generate novel transgenic and genetic models to define precisely when and where Smad-dependent signaling functions in different hemato-vascular progenitor populations. 2. Delineate the specificity of Smadl and SmadS for hematopoiesis. We will determine why the closely related BMP pathway mediators Smadl and SmadS have distinct regulatory functions with respect to hemato-vascular development. 3. Determine the molecular mechanisms by which Smad function regulates hematopoiesis. We propose to define the specificity, the pathways that are the targets for this activity, and the epigenetic changes that occur with respect to a key target gene, Gata2. Relevance to public health: Growth factors such as BMPs can regulate stem cell activity but their use in the clinic will not be feasible until we can accurately predict how they affect genetic programs in different progenitor cells. Our experiments should help to define the specificity of an important stem and progenitor cell regulatory pathway that is controlled in blood cells by BMPs.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37HL056182-13
Application #
7647950
Study Section
Hematopoiesis Study Section (HP)
Program Officer
Qasba, Pankaj
Project Start
1997-07-01
Project End
2010-02-28
Budget Start
2009-07-01
Budget End
2010-02-28
Support Year
13
Fiscal Year
2009
Total Cost
$251,301
Indirect Cost

  Institution

Name
Albert Einstein College of Medicine
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
110521739
City
Bronx
State
NY
Country
United States
Zip Code
10461

  Publications

Feng, Lingling; Cook, Brandoch; Tsai, Su-Yi et al. (2016) Discovery of a Small-Molecule BMP Sensitizer for Human Embryonic Stem Cell Differentiation. Cell Rep 15:2063-75
Sundaravel, Sriram; Duggan, Ryan; Bhagat, Tushar et al. (2015) Reduced DOCK4 expression leads to erythroid dysplasia in myelodysplastic syndromes. Proc Natl Acad Sci U S A 112:E6359-68
Gordillo, Miriam; Evans, Todd; Gouon-Evans, Valerie (2015) Orchestrating liver development. Development 142:2094-108
Mendelson, Karen; Lan, Yahui; Hla, Timothy et al. (2015) Maternal or zygotic sphingosine kinase is required to regulate zebrafish cardiogenesis. Dev Dyn 244:948-54
Li, Cheng; Lan, Yahui; Schwartz-Orbach, Lianna et al. (2015) Overlapping Requirements for Tet2 and Tet3 in Normal Development and Hematopoietic Stem Cell Emergence. Cell Rep 12:1133-43
Li, Xi; Lu, Yi-Chien; Dai, Kezhi et al. (2014) Elavl1a regulates zebrafish erythropoiesis via posttranscriptional control of gata1. Blood 123:1384-92
Das, Bhaskar C; Thapa, Pritam; Karki, Radha et al. (2014) Retinoic acid signaling pathways in development and diseases. Bioorg Med Chem 22:673-83
Cook, Brandoch D; Evans, Todd (2014) BMP signaling balances murine myeloid potential through SMAD-independent p38MAPK and NOTCH pathways. Blood 124:393-402
Choudhuri, Avik; Maitra, Umadas; Evans, Todd (2013) Translation initiation factor eIF3h targets specific transcripts to polysomes during embryogenesis. Proc Natl Acad Sci U S A 110:9818-23
Kumar, Ritu; DiMenna, Lauren; Schrode, Nadine et al. (2013) AID stabilizes stem-cell phenotype by removing epigenetic memory of pluripotency genes. Nature 500:89-92

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