Evidence for a Triplex DNA Conformation at the bcl-2 Major Breakpoint Region of the t(14;18) Translocation
The most common chromosomal translocation in cancer, t(14;18), occurs at the bcl-2 major breakpoint region (Mbr) in follicular lymphomas. The 150-bp bcl-2 Mbr, which contains three breakage hotspots (peaks), has a single-stranded character and, hence, a non-B DNA conformation both in vivo and in vit...
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Veröffentlicht in: | The Journal of biological chemistry 2005-06, Vol.280 (24), p.22749-22760 |
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Sprache: | eng |
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Zusammenfassung: | The most common chromosomal translocation in cancer, t(14;18), occurs at the bcl-2 major breakpoint region (Mbr) in follicular
lymphomas. The 150-bp bcl-2 Mbr, which contains three breakage hotspots (peaks), has a single-stranded character and, hence,
a non-B DNA conformation both in vivo and in vitro . Here, we use gel assays and electron microscopy to show that a triplex-specific antibody binds to the bcl-2 Mbr in vitro . Bisulfite reactivity shows that the non-B DNA structure is favored by, but not dependent upon, supercoiling and suggests
a possible triplex conformation at one portion of the Mbr (peak I). We have used circular dichroism to test whether the predicted
third strand of that suggested structure can indeed form a triplex with the duplex at peak I, and it does so with 1:1 stoichiometry.
Using an intracellular minichromosomal assay, we show that the non-B DNA structure formation is critical for the breakage
at the bcl-2 Mbr, because a 3-bp mutation that disrupts the putative peak I triplex also markedly reduces the recombination
of the Mbr. A three-dimensional model of such a triplex is consistent with bond length, bond angle, and energetic restrictions
(stacking and hydrogen bonding). We infer that an imperfect purine/purine/pyrimidine ( R. R.Y) triplex likely forms at the bcl-2 Mbr in vitro , and in vivo recombination data favor this as the major DNA conformation in vivo as well. |
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ISSN: | 0021-9258 1083-351X |
DOI: | 10.1074/jbc.M502952200 |