1997
DOI: 10.1128/mcb.17.7.4070
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DNA Cleavage within the MLL Breakpoint Cluster Region Is a Specific Event Which Occurs as Part of Higher-Order Chromatin Fragmentation during the Initial Stages of Apoptosis

Abstract: A distinct population of therapy-related acute myeloid leukemia (t-AML) is strongly associated with prior administration of topoisomerase II (topo II) inhibitors. These t-AMLs display distinct cytogenetic alterations, most often disrupting the MLL gene on chromosome 11q23 within a breakpoint cluster region (bcr) of 8.3 kb. We recently identified a unique site within the MLL bcr that is highly susceptible to DNA double-strand cleavage by classic topo II inhibitors (e.g., etoposide and doxorubicin). Here, we rep… Show more

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Cited by 170 publications
(177 citation statements)
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“…Cytostatic agents belonging to the topoisomerase II inhibitors interfere with rejoining of these double-strand breaks, and this activity is believed in some way to increase the risk of two simultaneous, illegitimate recombinations between the broken DNA strands of adjacent chromosomes. Studies of the genomic break-points of cases belonging to pathways III-VI now support this hypothesis, 39,[57][58][59][60][61] as the break points colocalize with topoisomerase II breakage sites.…”
Section: Origin Of Chromosome Aberrations and Specific Mutations In Tmentioning
confidence: 65%
“…Cytostatic agents belonging to the topoisomerase II inhibitors interfere with rejoining of these double-strand breaks, and this activity is believed in some way to increase the risk of two simultaneous, illegitimate recombinations between the broken DNA strands of adjacent chromosomes. Studies of the genomic break-points of cases belonging to pathways III-VI now support this hypothesis, 39,[57][58][59][60][61] as the break points colocalize with topoisomerase II breakage sites.…”
Section: Origin Of Chromosome Aberrations and Specific Mutations In Tmentioning
confidence: 65%
“…Recent data further suggest the existence of a broad range of agents capable of activating signal pathways, that disrupt chromatin and lead to apoptosis if allowed to proceed to completion. When interrupted prematurely, these signal pathways may produce translocations and thus allow the cell to escape the apoptotic fate (Stanulla et al, 1997b). Conceivably, these agents cleave chromatin at preferred sites, which may provide another explanation for the observed tight clustering of the translocation breakpoints in both genes.…”
Section: Discussionmentioning
confidence: 99%
“…It is clear that genomic MLL is a target of site-specific cleavage at the intron 11/exon 12 border in a variety of human cells. 7,8,10 As shown in Figures 2 and 3, both the entire 8.3 kbp MLL BCR and smaller fragments of 367 and 780 bp were subject to cleavage when placed as episomes in cells that were subsequently triggered to undergo apoptosis. Of note, all episomal inserts that supported cleavage contained both a strong topoisomerase II consensus binding site (at 6864-6847 as noted in Broeker et al 16 ) and the target for apoptotic cleavage at 6768 bp (see Figure 3).…”
Section: Discussionmentioning
confidence: 99%
“…In particular, therapy-related breakpoints appear clustered towards the telomeric region of the BCR, a region that colocalizes with a DNase I hypersensitivity site and is also a target for site-specific cleavage induced by apoptotic agents. [7][8][9] We have demonstrated before that cells exposed to triggers of the apoptotic program may initiate MLL cleavage and subsequent translocation, within cells that have the potential to divide. 10 In addition, direct analysis has shown that the cleavage event is linked to the release of high molecular weight (B50 kbp) DNA fragments, an early event in apoptosis execution.…”
Section: Introductionmentioning
confidence: 99%