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1 June 2005 DNA sequence determinants of nuclear protein binding to the c-Ha-ras antioxidant/electrophile response element in vascular smooth muscle cells: identification of Nrf2 and heat shock protein 90β as heterocomplex components
Kimberly P. Miller, Kenneth S. Ramos
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Abstract

The antioxidant/electrophile response element (ARE/EpRE) is a cis-acting element involved in redox regulation of c-Ha-ras gene. Protein binding to the ARE/EpRE may be credited to deoxyribonucleic acid sequence; therefore, studies were conducted to evaluate the influence of internal and flanking regions to the 10-bp human c-Ha-ras ARE/ EpRE core (hHaras10) on nuclear protein binding in oxidant-treated vascular smooth muscle cells. A protein doublet bound to an extended oligonucleotide comprising the ARE/EpRE core in genomic context (hHaras27), whereas a single complex bound to hHaras10. Protein binding involved specific interactions of 25- and 23-kDa proteins with hHaras10, and binding of 80-, 65-, and 55-kDa proteins to hHaras27. Competition assays with hNQO1 and rGSTA2 confirmed the specificity of deoxyribonucleic acid–protein interactions and indicated preferred binding of p25 and p23 to the c-Ha-ras ARE/EpRE. “NNN” sequences within the core afforded unique protein-binding profiles to the c-Ha-ras ARE/ EpRE. In addition, Nrf2 and heat shock protein 90β (p80) were identified as components of the c-Ha-ras ARE/EpRE heterocomplex. We conclude that both internal bases and flanking sequences regulate nuclear protein recruitment and complex assembly on the c-Ha-ras ARE/EpRE.

Kimberly P. Miller and Kenneth S. Ramos "DNA sequence determinants of nuclear protein binding to the c-Ha-ras antioxidant/electrophile response element in vascular smooth muscle cells: identification of Nrf2 and heat shock protein 90β as heterocomplex components," Cell Stress & Chaperones 10(2), 114-125, (1 June 2005). https://doi.org/10.1379/CSC-73R.1
Received: 9 August 2004; Accepted: 1 December 2004; Published: 1 June 2005
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