Abstract

This program is comprised of four highly interactive projects from Baylor College of Medicine (BCM) and M.D. Anderson Cancer Center (MDACC) in the Texas Medical Center (TMC) in Houston that focus on different aspects of the regulation of self-renewal and differentiation in human embryonic stem (hES) cells. The projects examine the role of and interactions between four proteins that have been shown to play a functional role in ES cells, namely nanog, Germ Cell Nuclear Factor (GCNF), the tumor suppressor protein p53, and a novel protein, THAP11. Our overall goal is to use this collaborative program project mechanism to understand how these proteins and the complexes with which they associate interact to regulate hES. Our program investigators have unique strengths in chromatin regulation, protein-protein interaction, gene repression, and hES biology that, when combined, will enable us to make a major contribution to the understanding of the regulation of pluripotency and differentiation in hES. Project 1 (Z. Songyang) involves study of proteins that interact with NANOG, and the mechanism through which NANOG represses genes involved in differentiation, particularly with regard to epigenetic regulation through the polycomb PRC1 complex. Project 2 (A. Cooney) is focused on the role of GCNF in repression of pluripotency genes, which is required for differentiation. Project 3 (M. Barton) focuses on p53, which has been shown to repress nanog in mouse ES cells. In Project 4 (T. Zwaka), THAP11 functions in hES will be examined. THAP11 has multiple features which potentially link epigenetic regulation of DNA and histones;THAP11 also can regulate suz12, a component of the PRC2 complex required for PRC1 activity, thus linking THAP11 with NANOG. The relevance of all these protein interactions for hES pluripotency and differentiation will be tested in multiple collaborative experiments. The projects will be supported by three cores. An Administrative Core will provide centralized support for all projects, and will also sponsor three pilot projects that will be competitively selected annually, enabling us to expand the number of investigators in the TMC who work with hES. We will sponsor a hES Training and Culture Core that will train TMC investigators in hES technologies in small bimonthly workshops. This core will also support the Projects and Pilot Project in hES maintenance, quality control and large-scale expansion. A Genetic Modification Core will offer tailored development of knock-in, knock-out, and tetracycline-regulated gene expression in hES cells. The overall program involves investigators from the University of Texas-Southwestern in Dallas as well as from BCM and MDACC. By bringing hES training and pilot grant funds into this region of the Southwest, our program will make hES technology accessible to a very large group of investigators and substantially strengthen hES expertise regionally.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Program Projects (P01)
Project #
5P01GM081627-04
Application #
7915188
Study Section
Special Emphasis Panel (ZGM1-GDB-8 (SC))
Program Officer
Zatz, Marion M
Project Start
2007-09-01
Project End
2012-08-31
Budget Start
2010-09-01
Budget End
2011-08-31
Support Year
4
Fiscal Year
2010
Total Cost
$1,557,723
Indirect Cost

  Institution

Name
Baylor College of Medicine
Department
Pediatrics
Type
Schools of Medicine
DUNS #
051113330
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Fujita, Jun; Freire, Pablo; Coarfa, Cristian et al. (2017) Ronin Governs Early Heart Development by Controlling Core Gene Expression Programs. Cell Rep 21:1562-1573
Jain, Abhinav K; Xi, Yuanxin; McCarthy, Ryan et al. (2016) LncPRESS1 Is a p53-Regulated LncRNA that Safeguards Pluripotency by Disrupting SIRT6-Mediated De-acetylation of Histone H3K56. Mol Cell 64:967-981
Wang, Hongran; Wang, Xiaohong; Xu, Xueping et al. (2016) Germ Cell Nuclear Factor (GCNF) Represses Oct4 Expression and Globally Modulates Gene Expression in Human Embryonic Stem (hES) Cells. J Biol Chem 291:8644-52
Wang, Hongran; Xi, Yutao; Zheng, Yi et al. (2016) Generation of electrophysiologically functional cardiomyocytes from mouse induced pluripotent stem cells. Stem Cell Res 16:522-30
Skinner, Samuel O; Xu, Heng; Nagarkar-Jaiswal, Sonal et al. (2016) Single-cell analysis of transcription kinetics across the cell cycle. Elife 5:e12175
Tang, Mengfan; Li, Yujing; Zhang, Yi et al. (2015) Disease mutant analysis identifies a new function of DAXX in telomerase regulation and telomere maintenance. J Cell Sci 128:331-41
Lu, Weisi; Fang, Lekun; Ouyang, Bin et al. (2015) Actl6a protects embryonic stem cells from differentiating into primitive endoderm. Stem Cells 33:1782-93
Zheng, Ze-Yi; Tian, Lin; Bu, Wen et al. (2015) Wild-Type N-Ras, Overexpressed in Basal-like Breast Cancer, Promotes Tumor Formation by Inducing IL-8 Secretion via JAK2 Activation. Cell Rep 12:511-24
Sabour, Davood; Xu, Xueping; Chung, Arthur C K et al. (2014) Germ cell nuclear factor regulates gametogenesis in developing gonads. PLoS One 9:e103985
Li, Yujing; Fong, Ka-Wing; Tang, Mengfan et al. (2014) Fam118B, a newly identified component of Cajal bodies, is required for Cajal body formation, snRNP biogenesis and cell viability. J Cell Sci 127:2029-39

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