Structural Basis for Stable DNA Complex Formation by the Caspase-activated DNase

Reh, Stefanie; Korn, Christian; Gimadutdinow, Oleg; Meiß, Gregor

doi:10.1074/jbc.m509133200

Cited by 12 publications

(13 citation statements)

References 42 publications

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“…The nuclease is inhibited by several poly-anions, like heparin, polyglutamic acid [66], poly(ADP-ribose) [67] and nucleic acids that are not its substrates (single stranded DNA, RNA and DNA-RNA heteroduplexes) [34,66]. Such polyanions, which are thought to bind to the positively charged surface formed by the a4 helices of DFF40 and impair its ability to bind to double-stranded DNA, are competitive inhibitors of the nuclease [66,68]. Knowing that RNA, which inhibits DFF40 in vitro, is the major cellular poly-anion, one could postulate that apoptotic chromatin breakdown might be coordinated with RNA degradation in vivo, and DFF activity would be kept in check until RNA levels fall below some inhibitory threshold.…”

Section: Effectors That Regulate Dffmentioning

confidence: 98%

Roles of the Major Apoptotic Nuclease-DNA Fragmentation Factor-in Biology and Disease

Widłak

Garrard

2008

Cell. Mol. Life Sci.

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It has now been more than ten years since the discovery of the major apoptotic nuclease, DNA fragmentation factor (DFF), also known as caspase-activated DNase (CAD). Here we review the recent literature that has uncovered new insight into DFF's regulation, and both its positive and negative roles in human disease. Cells from mice deficient in DFF still undergo apoptotic death without significant cell-autonomous DNA degradation. Their corpses' genomes are subsequently degraded by lysosomal DNase II after phagocytosis. However,DFF-deficient mice are more susceptible to cancer. Indeed, several different cancers in humans are associated with defects in DFF expression and it has been proposed that DFF is a p53-independent tumor suppressor. Negative aspects of DFF expression include contributing to susceptibility to acquire systemic lupus erythematosus, to chromosomal translocations that result in mixed lineage leukemias, and in the possible spreading of oncogenes and HIV due to horizontal gene transfer.

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Section: Effectors That Regulate Dffmentioning

confidence: 98%

Roles of the Major Apoptotic Nuclease-DNA Fragmentation Factor-in Biology and Disease

Widłak

Garrard

2008

Cell. Mol. Life Sci.

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“…11,12 Following translation the ICAD-L/CAD complex localizes to the nucleus, where it remains highly mobile; however, stable interactions with DNA have been noted suggesting that CAD can be activated not only in the free nuclear space but also in a DNA associated complex. [13][14][15] To activate CAD, caspase 3 targets ICAD for proteolytic cleavage at 2 aspartic acids, D117 and D224. This caspase directed cleavage destabilizes the ICAD/CAD interaction and allows CAD dimerization.…”

Section: Parole Terms For a Killermentioning

confidence: 99%

Parole terms for a killer

Larsen

Megeney²

2010

Cell Cycle

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“…4 A and B). Activated CAD as well as the CAD-ICAD complex has been shown to form stable complexes with substrate DNA, suggesting that ICAD may be cleaved by caspase 3 in this DNA-associated complex to activate CAD in a specific manner (12). This stable association allowed for ChIP with an antibody specific for CAD to precipitate associated genomic regions at 12 and 24 h postinduction of differentiation in C2C12 myoblasts.…”

mentioning

confidence: 99%

“…CAD is held in check through association with its inhibitor, inhibitor of caspase-activated DNase (ICAD), which is cleaved by caspase 3 to release CAD (10,11). After activation, unobstructed CAD configures into a scissor-like dimer, cleaving DNA with minimal sequence specificity (10,12). CAD is also ubiquitously expressed, suggesting a highly conserved function for this nuclease.…”

mentioning

confidence: 99%

Caspase 3/caspase-activated DNase promote cell differentiation by inducing DNA strand breaks

Larsen

Rampalli

Burns

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

217

204

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Caspase 3 is required for the differentiation of a wide variety of cell types, yet it remains unclear how this apoptotic protein could promote such a cell-fate decision. Caspase signals often result in the activation of the specific nuclease caspase-activated DNase (CAD), suggesting that cell differentiation may be dependent on a CADmediated modification in chromatin structure. In this study, we have investigated if caspase 3/CAD plays a role in initiating the DNA strand breaks that are known to occur during the terminal differentiation of skeletal muscle cells. Here, we show that inhibition of caspase 3 or reduction of CAD expression leads to a dramatic loss of strand-break formation and a block in the myogenic program. Caspase-dependent induction of differentiation results in CAD targeting of the p21 promoter, and loss of caspase 3 or CAD leads to a significant down-regulation in p21 expression. These results show that caspase 3/CAD promotes cell differentiation by directly modifying the DNA/nuclear microenvironment, which enhances the expression of critical regulatory genes.development | gene expression | non-apoptotic caspase activity | epigenetics

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Structural Basis for Stable DNA Complex Formation by the Caspase-activated DNase

Cited by 12 publications

References 42 publications

Roles of the Major Apoptotic Nuclease-DNA Fragmentation Factor-in Biology and Disease

Roles of the Major Apoptotic Nuclease-DNA Fragmentation Factor-in Biology and Disease

Parole terms for a killer

Caspase 3/caspase-activated DNase promote cell differentiation by inducing DNA strand breaks

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