Proapoptotic BID Is an ATM Effector in the DNA-Damage Response

Kamer, Iris; Sarig, Rachel; Zaltsman, Yehudit; Niv, Hagit; Oberkovitz, Galia; Regev, Limor; Haimovich, Gal; Lerenthal, Yaniv; Marcellus, Richard; Gross, Atan

doi:10.1016/j.cell.2005.06.014

Cited by 202 publications

(244 citation statements)

References 17 publications

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“…62 These abnormal chromosomal structures represent 'chromatid-type' errors, resulting from improperly repaired DNA damage accrued during S phase of the cell 62 Bid À/À myeloid progenitor cells and MEFs fail to properly execute the ionizing radiation-induced intra-S-phase checkpoint. 62,63 This Sphase role is mediated through BID phosphorylation at position 78 by the DNA damage kinase ATM, demonstrating a direct link between BID and the DNA damage response. These studies demonstrate that BID plays a novel role in preserving genomic integrity that places BID at an early point in the path to determine the fate of a cell (Figure 2).…”

Section: Proapoptotic Bidmentioning

confidence: 92%

“…Casein kinases have been implicated in BID phosphorylation, and ATM has been shown to phosphorylate BID following DNA damage. [61][62][63] Phosphorylated BID is resistant to caspase cleavage in in vitro assays, and MEFs harboring phosphorylation-defective S78A BID are more sensitive to etoposide-induced cell death. The above data are consistent with a role for phosphorylation to inhibit activation of BID's proapoptotic function.…”

Section: Proapoptotic Bidmentioning

confidence: 99%

“…The above data are consistent with a role for phosphorylation to inhibit activation of BID's proapoptotic function. 61,63 How might BID be involved in suppressing leukemogenesis? Although the loss of BID could theoretically reset death susceptibility in both intrinsic and extrinsic pathways, it is less obvious why the absence of BID should prove so oncogenic.…”

Section: Proapoptotic Bidmentioning

confidence: 99%

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BCL2 family in DNA damage and cell cycle control

2006

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Individual BCL2 family members couple apoptosis regulation and cell cycle control in unique ways. Antiapoptotic BCL2 and BCL-x L are antiproliferative by facilitating G0. BAX is proapoptotic and accelerates S-phase progression. The dual functions in apoptosis and cell cycle are coordinately regulated by the multi-domain BCL2 family members (MCL-1) and suggest that survival is maintained at the expense of proliferation. The role of BH3-only molecules in cell cycle is more variable. BAD antagonizes both the cell cycle and antiapoptotic functions of BCL2 and BCL-x L through BH3 binding. BID has biochemically separable functions in apoptosis and S-phase checkpoint, determined by posttranslational modification. p53-induced PUMA is known only to have apoptotic function. Inhibition of apoptosis is oncogenic, whereas promotion of cell cycle arrest is tumor suppressive. Paradoxically, selected BCL2 family members can be both oncogenic and tumor suppressive. Which of the dual functions predominates is lineage specific and context dependent.

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Section: Proapoptotic Bidmentioning

confidence: 92%

Section: Proapoptotic Bidmentioning

confidence: 99%

Section: Proapoptotic Bidmentioning

confidence: 99%

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BCL2 family in DNA damage and cell cycle control

2006

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“…57 In addition to these internal familybased interactions, BCL-2 proteins associate with a host of other cellular proteins 31,47,[63][64][65][66][67][68][69][70][71] and have emerging roles in diverse physiologic pathways including glucose metabolism 20 and the DNA-damage response. 24,40 …”

Section: Introductionmentioning

confidence: 99%

BCL-2 in the crosshairs: tipping the balance of life and death

Walensky¹

2006

Cell Death Differ

225

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The discovery of B-cell lymphoma-2 (BCL-2) over 20 years ago revealed a new paradigm in cancer biology: the development and persistence of cancer can be driven by molecular roadblocks along the natural pathway to cell death. The subsequent identification of an expansive family of BCL-2 proteins provoked an intensive investigation of the interplay among these critical regulators of cell death. What emerged was a compelling tale of guardians and executioners, each participating in a molecular choreography that dictates cell fate. Ten years into the BCL-2 era, structural details defined how certain BCL-2 family proteins interact, and molecular targeting of the BCL-2 family has since become a pharmacological quest. Although many facets of BCL-2 family death signaling remain a mechanistic mystery, small molecules and peptides that effectively target BCL-2 are eliminating the roadblock to cell death, raising hopes for a medical breakthrough in cancer and other diseases of deregulated apoptosis.

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“…1 Previously we have reported that DNA damage induces the phosphorylation of BID on serines 61 and 78 by the ataxia-telangiectasia mutated (ATM) kinase, and that this phosphorylation is important for cell cycle arrest and inhibition of apoptosis. 2 In addition, another group reported similar results in response to replicative stress. 3 Nevertheless, these findings were challenged by a third group, which demonstrated that in response to DNA damage BID −/− cells underwent cell cycle arrest and apoptosis in a manner indistinguishable from wild-type cells, arguing that BID is dispensable for the DDR.…”

mentioning

confidence: 81%

The ATM–BID pathway plays a critical role in the DNA damage response by regulating mitochondria metabolism

2015

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We are writing this correspondence as an attempt to resolve controversy in the field regarding the role of BID in the DNA damage response (DDR). BID is a well-established BH3-only BCL-2 family member that has a critical role in regulating mitochondrial apoptosis. 1 Previously we have reported that DNA damage induces the phosphorylation of BID on serines 61 and 78 by the ataxia-telangiectasia mutated (ATM) kinase, and that this phosphorylation is important for cell cycle arrest and inhibition of apoptosis. 2 In addition, another group reported similar results in response to replicative stress. 3 Nevertheless, these findings were challenged by a third group, which demonstrated that in response to DNA damage BID −/− cells underwent cell cycle arrest and apoptosis in a manner indistinguishable from wild-type cells, arguing that BID is dispensable for the DDR. 4 This study did not however touch upon the connection between BID and ATM. Thus, the role of BID in the DDR in the minds of many was not resolved.In an endeavour to resolve these differences and advance our knowledge, we generated BID S61A/S78A (BID AA ) knock-in mice, in which endogenous BID is no longer capable of being phosphorylated by ATM. We found that BID AA mice are hypersensitive to whole-body irradiation and that this hypersensitivity was due to premature entry of haematopoietic stem cells (HSC) into active cell cycle and increased levels of HSC apoptosis. 5 We also demonstrated that loss of BID phosphorylation was associated with accumulation of BID at the mitochondria and elevated levels of mitochondrial reactive oxygen species (ROS), suggesting that basal phosphorylation of BID is critical for balancing mitochondrial ROS, thus regulating HSC quiescence.Interestingly, BID −/− mice are not hypersensitive to DNA damage and show no abnormal HSC phenotypes in steady state or stress-induced haematopoiesis. 5 This is most likely due to the fact that deletion of BID attenuates overproduction of mitochondrial ROS, maintaining normal basal ROS. Therefore, BID −/− mice are not expected to have the same phenotypes as BID AA mice. The differential sensitivity between these two mouse models in response to DNA damage supports the notion and explains the initial alleged contradiction that the changes in baseline ROS level per se rather than BID itself dictate the sensitivity to DNA damage. Thus, the new BID AA mouse model helped us shed new light upon this controversy and demonstrated that BID does have a critical role in the DDR in vivo.Our more recent findings suggest that BID regulates mitochondrial ROS/metabolism via mitochondrial carrier homolog 2 (MTCH2). MTCH2 acts as a mitochondrial receptor for BID essential for apoptosis, 6 and is suspected to have a role in metabolism. 7 Importantly, we recently found that loss of MTCH2 in the haematopoietic system results in premature entry of HSCs into cycle accompanied by a moderate increase in mitochondrial ROS, 8 findings that were similar to the ones obtained with the BID AA mice. Moreover, loss of MTCH2 or loss ...

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Proapoptotic BID Is an ATM Effector in the DNA-Damage Response

Cited by 202 publications

References 17 publications

BCL2 family in DNA damage and cell cycle control

BCL2 family in DNA damage and cell cycle control

BCL-2 in the crosshairs: tipping the balance of life and death

The ATM–BID pathway plays a critical role in the DNA damage response by regulating mitochondria metabolism

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