Abstract

The objective of this program is to understand the regulation of the cell cycle dependent human histone genes, a multi-gene family of moderately repeated sequences with differences in the structure, organization and regulation of the various copies. The tight coupling of histone gene expression with DNA replication and the stringent requirement of histones to package newly replicated DNA into nucleosomes account for the involvement of histone gene expression in control of cell growth and cell division. Studies carried out during the current funding period have identified sequences that influence specificity, level and cell cycle regulation of histone gene transcription and have confirmed the modular organization of histone gene promoters. A series of proximal and distal H4 histone promoter elements have been examined by deletion analysis, site directed mutagenesis and construction of chimeric genes assayed in vitro, by transfection into mammalian cells and in transgenic mice. Protein-DNA interactions in the proximal promoter have been established in intact cells at single nucleotide resolution and several nuclear protein factors have been characterized in vitro. In vitro protein-DNA interactions with the most proximal promoter element have been shown to be stringently cell cycle controlled in diploid cells and deregulated (constitutive) in transformed and tumor cells where loss of binding occurs only with the onset of differentiation. These results serve as the basis for ongoing and proposed studies which are: 1) To further define and characterize sequences in histone gene promoters that modulate levels of transcription during the cell cycle and are responsible for the downregulation of transcription during differentiation; 2) To continue the identification and characterization of protein-DNA interactions in intact cells in the 5' promoter of a histone gene; 3) To isolate and characterize promoter binding factors that interact with proximal and distal 5' regulatory elements; 4) To assess the contributions of factor regulation to the control of histone gene transcription by a) determining the role of phosphorylation in factor- regulatory sequence interactions, and b) cloning cDNAs for histone gene promoter binding factors to determine the extent to which their regulation influences histone gene transcription; and 5) To examine the potential involvement of nuclear structure with the regulation of histone gene expression by determining the relationship of histone gene transcription to nuclear matrix association of the genes and by exploring the possibility that the nuclear matrix may concentrate and/or localize histone promoter binding factors.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM032010-11
Application #
3280543
Study Section
Physiological Chemistry Study Section (PC)
Project Start
1987-09-01
Project End
1995-03-31
Budget Start
1992-04-01
Budget End
1993-03-31
Support Year
11
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
University of Massachusetts Medical School Worcester
Department
Type
Schools of Medicine
DUNS #
660735098
City
Worcester
State
MA
Country
United States
Zip Code
01655

  Publications

Stein, Gary S; Stein, Janet L; van J Wijnen, Andre et al. (2012) The architectural organization of human stem cell cycle regulatory machinery. Curr Pharm Des 18:1679-85
Zaidi, Sayyed K; Medina, Ricardo F; Pockwinse, Shirwin M et al. (2010) Subnuclear localization and intranuclear trafficking of transcription factors. Methods Mol Biol 647:77-93
Xie, Ronglin; Medina, Ricardo; Zhang, Ying et al. (2009) The histone gene activator HINFP is a nonredundant cyclin E/CDK2 effector during early embryonic cell cycles. Proc Natl Acad Sci U S A 106:12359-64
Mitra, Partha; Ghule, Prachi N; van der Deen, Margaretha et al. (2009) CDK inhibitors selectively diminish cell cycle controlled activation of the histone H4 gene promoter by p220NPAT and HiNF-P. J Cell Physiol 219:438-48
Ghule, Prachi N; Dominski, Zbigniew; Lian, Jane B et al. (2009) The subnuclear organization of histone gene regulatory proteins and 3' end processing factors of normal somatic and embryonic stem cells is compromised in selected human cancer cell types. J Cell Physiol 220:129-35
Filion, Tera M; Qiao, Meng; Ghule, Prachi N et al. (2009) Survival responses of human embryonic stem cells to DNA damage. J Cell Physiol 220:586-92
Medina, Ricardo; Buck, Timothy; Zaidi, Sayyed K et al. (2008) The histone gene cell cycle regulator HiNF-P is a unique zinc finger transcription factor with a novel conserved auxiliary DNA-binding motif. Biochemistry 47:11415-23
Pockwinse, Shirwin M; Zaidi, Sayyed K; Medina, Ricardo F et al. (2008) In situ nuclear organization of regulatory machinery. Methods Mol Biol 455:239-59
Medina, Ricardo; Zaidi, Sayyed K; Liu, Chang-Gong et al. (2008) MicroRNAs 221 and 222 bypass quiescence and compromise cell survival. Cancer Res 68:2773-80
Ghule, Prachi N; Dominski, Zbigniew; Yang, Xiao-Cui et al. (2008) Staged assembly of histone gene expression machinery at subnuclear foci in the abbreviated cell cycle of human embryonic stem cells. Proc Natl Acad Sci U S A 105:16964-9

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