Overlapping and CpG methylation-sensitive protein-DNA interactions at the histone H4 transcriptional cell cycle domain: distinctions between two human H4 gene promoters.

This Article

	Full Text (PDF)
	Alert me when this article is cited
	Alert me if a correction is posted

Services

	Similar articles in this journal
	Similar articles in PubMed
	Alert me to new issues of the journal
	Download to citation manager
	Reprints and Permissions
	Copyright Information
	Books from ASM Press
	MicrobeWorld

Citing Articles

	Citing Articles via HighWire
	Citing Articles via Google Scholar

Google Scholar

	Articles by van Wijnen, A J
	Articles by Stein, G S
	Search for Related Content

PubMed

	PubMed Citation
	Articles by van Wijnen, A J
	Articles by Stein, G S

Previous Article | Next Article

Mol Cell Biol. 1992 July; 12(7): 3273-3287

Overlapping and CpG methylation-sensitive protein-DNA interactions at the histone H4 transcriptional cell cycle domain: distinctions between two human H4 gene promoters.

A J van Wijnen, F M van den Ent, J B Lian, J L Stein and G S Stein

Department of Cell Biology, University of Massachusetts Medical Center, Worcester 01655.

ABSTRACT

Transcriptional regulation of vertebrate histone genes duringthe cell cycle is mediated by several factors interacting witha series of cis-acting elements located in the 5' regions ofthese genes. The arrangement of these promoter elements is differentfor each gene. However, most histone H4 gene promoters containa highly conserved sequence immediately upstream of the TATAbox (H4 subtype consensus sequence), and this region in thehuman H4 gene FO108 is involved in cell cycle control. The sequence-specificinteraction of nuclear factor HiNF-D with this key proximalpromoter element of the H4-FO108 gene is cell cycle regulatedin normal diploid cells (J. Holthuis, T.A. Owen, A.J. van Wijnen,K.L. Wright, A. Ramsey-Ewing, M.B. Kennedy, R. Carter, S.C.Cosenza, K.J. Soprano, J.B. Lian, J.L. Stein, and G.S. Stein,Science, 247:1454-1457, 1990). Here, we show that this regionof the H4-FO108 gene represents a composite protein-DNA interactiondomain for several distinct sequence-specific DNA-binding activities,including HiNF-D, HiNF-M, and HiNF-P. Factor HiNF-P is similarto H4TF-2, a DNA-binding activity that is not cell cycle regulatedand that interacts with the analogous region of the H4 geneH4.A (F. LaBella and N. Heintz, Mol. Cell. Biol. 11:5825-5831,1991). The H4.A gene fails to interact with factors HiNF-M andHiNF-D owing to two independent sets of specific nucleotidevariants, indicating differences in protein-DNA interactionsbetween these H4 genes. Cytosine methylation of a highly conservedCpG dinucleotide interferes with binding of HiNF-P/H4TF-2 toboth the H4-FO108 and H4.A promoters, but no effect is observedfor either HiNF-M or HiNF-D binding to the H4-FO108 gene. Thus,strong evolutionary conservation of the H4 consensus sequencemay be related to combinatorial interactions involving overlappingand interdigitated recognition nucleotides for several proteins,whose activities are regulated independently. Our results alsosuggest molecular complexity in the transcriptional regulationof distinct human H4 genes.

Mol Cell Biol. 1992 July; 12(7): 3273-3287

This article has been cited by other articles:

Medina, R., van der Deen, M., Miele-Chamberland, A., Xie, R.-L., van Wijnen, A. J., Stein, J. L., Stein, G. S. (2007). The HiNF-P/p220NPAT Cell Cycle Signaling Pathway Controls Nonhistone Target Genes. Cancer Res. 67: 10334-10342 [Abstract] [Full Text]
Eirin-Lopez, J. M., Lewis, J. D., Howe, L. A., Ausio, J. (2006). Common Phylogenetic Origin of Protamine-like (PL) Proteins and Histone H1: Evidence from Bivalve PL Genes. Mol Biol Evol 23: 1304-1317 [Abstract] [Full Text]
Holmes, W. F., Braastad, C. D., Mitra, P., Hampe, C., Doenecke, D., Albig, W., Stein, J. L., van Wijnen, A. J., Stein, G. S. (2005). Coordinate Control and Selective Expression of the Full Complement of Replication-dependent Histone H4 Genes in Normal and Cancer Cells. J. Biol. Chem. 280: 37400-37407 [Abstract] [Full Text]
Miele, A., Braastad, C. D., Holmes, W. F., Mitra, P., Medina, R., Xie, R., Zaidi, S. K., Ye, X., Wei, Y., Harper, J. W., van Wijnen, A. J., Stein, J. L., Stein, G. S. (2005). HiNF-P Directly Links the Cyclin E/CDK2/p220NPAT Pathway to Histone H4 Gene Regulation at the G1/S Phase Cell Cycle Transition. Mol. Cell. Biol. 25: 6140-6153 [Abstract] [Full Text]
Chowdhary, R., Ali, R. A., Albig, W., Doenecke, D., Bajic, V. B (2005). Promoter modeling: the case study of mammalian histone promoters. Bioinformatics 21: 2623-2628 [Abstract] [Full Text]
Mitra, P., Xie, R.-L., Medina, R., Hovhannisyan, H., Zaidi, S. K., Wei, Y., Harper, J. W., Stein, J. L., van Wijnen, A. J., Stein, G. S. (2003). Identification of HiNF-P, a Key Activator of Cell Cycle-Controlled Histone H4 Genes at the Onset of S Phase. Mol. Cell. Biol. 23: 8110-8123 [Abstract] [Full Text]
Xie, R.-L., Gupta, S., Miele, A., Shiffman, D., Stein, J. L., Stein, G. S., van Wijnen, A. J. (2003). The Tumor Suppressor Interferon Regulatory Factor 1 Interferes with SP1 Activation to Repress the Human CDK2 Promoter. J. Biol. Chem. 278: 26589-26596 [Abstract] [Full Text]
Hovhannisyan, H., Cho, B., Mitra, P., Montecino, M., Stein, G. S., van Wijnen, A. J., Stein, J. L. (2003). Maintenance of Open Chromatin and Selective Genomic Occupancy at the Cell Cycle-Regulated Histone H4 Promoter during Differentiation of HL-60 Promyelocytic Leukemia Cells. Mol. Cell. Biol. 23: 1460-1469 [Abstract] [Full Text]
Xie, R.-L., van Wijnen, A. J., van der Meijden, C. M., Stein, J. L., Stein, G. S. (2002). Forced Expression of the Interferon Regulatory Factor 2 Oncoprotein Causes Polyploidy and Cell Death in FDC-P1 Myeloid Hematopoietic Progenitor Cells. Cancer Res. 62: 2510-2515 [Abstract] [Full Text]
Singal, R., vanWert, J., Bashambu, M., Wolfe, S. A., Wilkerson, D. C., Grimes, S. R. (2000). Testis-Specific Histone H1t Gene Is Hypermethylated in Nongerminal Cells in the Mouse. Biol. Reprod. 63: 1237-1244 [Abstract] [Full Text]
Lemercier, C., Duncliffe, K., Boibessot, I., Zhang, H., Verdel, A., Angelov, D., Khochbin, S. (2000). Involvement of Retinoblastoma Protein and HBP1 in Histone H10 Gene Expression. Mol. Cell. Biol. 20: 6627-6637 [Abstract] [Full Text]
Zhao, J., Kennedy, B. K., Lawrence, B. D., Barbie, D. A., Matera, A. G., Fletcher, J. A., Harlow, E. (2000). NPAT links cyclin E-Cdk2 to the regulation of replication-dependent histone gene transcription. Genes Dev. 14: 2283-2297 [Abstract] [Full Text]
van Gurp, M. F., Pratap, J., Luong, M., Javed, A., Hoffmann, H., Giordano, A., Stein, J. L., Neufeld, E. J., Lian, J. B., Stein, G. S., van Wijnen, A. J. (1999). The CCAAT Displacement Protein/cut Homeodomain Protein Represses Osteocalcin Gene Transcription and Forms Complexes with the Retinoblastoma Protein-related Protein p107 and Cyclin A. Cancer Res. 59: 5980-5988 [Abstract] [Full Text]
Vaughan, P. S., van der Meijden, C. M.�J., Aziz, F., Harada, H., Taniguchi, T., van Wijnen, A. J., Stein, J. L., Stein, G. S. (1998). Cell Cycle Regulation of Histone H4 Gene Transcription Requires the Oncogenic Factor IRF-2. J. Biol. Chem. 273: 194-199 [Abstract] [Full Text]
Xie, R., van Wijnen, A. J., van der Meijden, C., Luong, M. X., Stein, J. L., Stein, G. S. (2001). The Cell Cycle Control Element of Histone H4 Gene Transcription Is Maximally Responsive to Interferon Regulatory Factor Pairs IRF-1/IRF-3 and IRF-1/IRF-7. J. Biol. Chem. 276: 18624-18632 [Abstract] [Full Text]

J. Bacteriol.	J. Virol.	Eukaryot. Cell

Microbiol. Mol. Biol. Rev.	Clin. Vaccine Immunol.	All ASM Journals