Your browser version may not work well with NCBI's Web applications. More information here...
1: Bioorg Med Chem Lett. 2006 Dec 15;16(24):6161-4. Epub 2006 Sep 29.Click here to read Links

Binding of f-PIP, a pyrrole- and imidazole-containing triamide, to the inverted CCAAT box-2 of the topoisomerase IIalpha promoter and modulation of gene expression in cells.

Le NM, Sielaff AM, Cooper AJ, Mackay H, Brown T, Kotecha M, O'Hare C, Hochhauser D, Lee M, Hartley JA.

Department of Chemistry, Furman University, 3300 Pointsett Highway, Greenville, SC 29613, USA.

An N-formamido pyrrole- and imidazole-containing triamide (f-PIP) has been shown by DNase I footprinting, SPR, and CD studies to bind as a stacked dimer to its cognate sequences: 5'-TACGAT-3' (5'-flank of the inverted CCAAT box-2 of the human topoisomerase IIalpha promoter) and 5'-ATCGAT-3'. A gel shift experiment provided evidence for f-PIP to inhibit protein-DNA interaction at the ICB2 site. Western blot studies showed that expression of the topoisomerase IIalpha gene in confluent NIH 3T3 cells was induced by treatment with f-PIP. The results suggested that the triamide was able to enter the nucleus, interacted with the target site within ICB2, inhibited NF-Y binding, and activated gene expression.

PMID: 17011187 [PubMed - indexed for MEDLINE]