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Science 5 June 1987:
Vol. 236. no. 4806, pp. 1308 - 1311
DOI: 10.1126/science.3035717
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Articles

Science, Vol 236, Issue 4806, 1308-1311
Copyright © 1987 by American Association for the Advancement of Science

articles

Protein-DNA interactions in vivo upstream of a cell cycle-regulated human H4 histone gene

U Pauli, S Chrysogelos, G Stein, J Stein, and H Nick

Cell cycle-dependent histone genes are transcribed at a basal level throughout the cell cycle, with a three- to fivefold increase during early S phase. Protein-DNA interactions in the 5' promoter region of a cell cycle-regulated human H4 histone gene have been analyzed at single-nucleotide resolution in vivo. This region contains two sites, with four potential protein-binding domains, at which the DNA is protected from reaction with dimethyl sulfate in cells and from digestion with deoxyribonuclease I in nuclei. These protein-DNA interactions persist during all phases of the cell cycle and dissociate with 0.16 to 0.2M sodium chloride.


THIS ARTICLE HAS BEEN CITED BY OTHER ARTICLES:
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Coordinate Control and Selective Expression of the Full Complement of Replication-dependent Histone H4 Genes in Normal and Cancer Cells.
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HiNF-P Directly Links the Cyclin E/CDK2/p220NPAT Pathway to Histone H4 Gene Regulation at the G1/S Phase Cell Cycle Transition.
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Identification of HiNF-P, a Key Activator of Cell Cycle-Controlled Histone H4 Genes at the Onset of S Phase.
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Role for a YY1-Binding Element in Replication-Dependent Mouse Histone Gene Expression.
K. A. Eliassen, A. Baldwin, E. M. Sikorski, and M. M. Hurt (1998)
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Tumor cells exhibit deregulation of the cell cycle histone gene promoter factor HiNF-D.
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Purification of the human histone H4 gene-specific transcription factors H4TF-1 and H4TF-2..
L Dailey, S B Roberts, and N Heintz (1988)
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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.
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J. Biol. Chem. 276, 18624-18632
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Science. ISSN 0036-8075 (print), 1095-9203 (online)