Activation of Calpain I Converts Excitotoxic Neuron Death into a Caspase-independent Cell Death

Lankiewicz, Silke; Luetjens, C. Marc; Bui, Nguyen Truc; Krohn, Aaron J.; Poppe, Monika; Cole, Greg M.; Saido, Takaomi C.; Prehn, Jochen H.M.

doi:10.1074/jbc.275.22.17064

Cited by 255 publications

(234 citation statements)

References 55 publications

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“…Accordingly, caspase-3 underwent cleavage into a 17-kDa active form that could be identified by immunoblot from 24 h of starving. An additional 29-kDa band, previously described as a calpainmediated breakdown product, 21,34 was detectable at 96 h, suggesting crosstalk between these two families of proteases ( Figure 2b). We also determined the activation status of caspase-12, an endoplasmic reticulum-associated caspase, previously related to serum deprivation-induced apoptosis in other systems.…”

Section: Apoptosis Of 661w Cells Proceeds With Participation Of Caspasesmentioning

confidence: 65%

Multiple death pathways in retina-derived 661W cells following growth factor deprivation: crosstalk between caspases and calpains

2005

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During development of the mammalian retina, neurons that do not succeed in establishing functional synaptic connections are eliminated by apoptosis, allowing the formation of a finely tuned network. Growth factors play a crucial role in controlling the balance between apoptosis and survival signals not only at developmental stages but also in longterm preservation of retinal functions. In the present work, we explore the apoptotic mechanisms triggered by growth factor deprivation of retina-derived 661W cells. Under serum starvation conditions, these cone photoreceptors underwent cell death with participation of caspase-9, -3 and -12. Interestingly, inhibition of caspases did not prevent apoptosis but only resulted in a temporary delay. We show m-calpain activation in parallel with caspases, indicating that more than one execution pathway is available to cone photoreceptors. Moreover, crosstalk of the caspase and calpain pathways was detected, suggesting a loop that may act to amplify the apoptotic cascade.

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Section: Apoptosis Of 661w Cells Proceeds With Participation Of Caspasesmentioning

confidence: 65%

Multiple death pathways in retina-derived 661W cells following growth factor deprivation: crosstalk between caspases and calpains

2005

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“…Calpains have been shown to be often associated with caspase activation in different apoptotic pathways (Neumar et al, 2003;Altznauer et al, 2004). However, caspase-independent cell death mediated by calpains has also been described in several models, including neuronal cell death (Lankiewicz et al, 2000) and vitamine-D-induced apoptosis in breast cancer cells (Mathiasen et al, 2002). Although calpain has a large number of substrates, its exact role in cell death remains unclear.…”

Section: Discussionmentioning

confidence: 99%

CD44 ligation induces caspase-independent cell death via a novel calpain/AIF pathway in human erythroleukemia cells

et al. 2006

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Ligation of the cell surface molecule CD44 by anti-CD44 monoclonal antibodies (mAbs) has been shown to induce cell differentiation, cell growth inhibition and in some cases, apoptosis in myeloid leukemic cells. We report, herein, that exposure of human erythroleukemic HEL cells to the anti-CD44 mAb A3D8 resulted in cell growth inhibition followed by caspase-independent apoptosis-like cell death. This process was associated with the disruption of mitochondrial membrane potential (DWm), the mitochondrial release of apoptosis-inducing factor (AIF), but not of cytochrome c, and the nuclear translocation of AIF. All these effects including cell death, loss of mitochondrial DWm and AIF release were blocked by pretreatment with the poly (ADP-ribose) polymerase inhibitor isoquinoline. A significant protection against cell death was also observed by using small interfering RNA for AIF. Moreover, we show that calpain protease was activated before the appearance of apoptosis, and that calpain inhibitors or transfection of calpain-siRNA decrease A3D8-induced cell death, and block AIF release. These data suggest that CD44 ligation triggers a novel caspaseindependent cell death pathway via calpain-dependent AIF release in erythroleukemic HEL cells.

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“…27 In the same way, RARaÀ/À mice exhibit caspase-independent spermatid loss. 28 Late differentiating male germ cells share similarities with various postmitotic/terminally differentiating models of caspase-independent cell death: p53-expressing or NMDAtreated neurons, 17,18 ischemic mature brain, 29 light-injured mature photoreceptor cells 19 or differentiating PC12 cells. 30 So in terminally maturing cells, calpain activation bypasses an inhibition or a block in the caspase pathway generally related to a decrease in apoptotic effectors like Apaf1 or caspase-3.…”

Section: Discussionmentioning

confidence: 99%

“…These ubiquitous enzymes are involved (i) in testicular cell loss in ischemia/reperfusion models, 6 and (ii) in several models of postmitotic, differentiating cell death. [17][18][19] Calpain 2 mRNAs were observed at all differentiation stages of normal spermatogenesis without any modification in transgenic cells (Figure 7a). By contrast, calpain 1 mRNAs were only detected in normal SP cells and spermatocytes II.…”

Section: Calpains Are the Main Protease Effectors Of Death In Mtp53 Gmentioning

confidence: 94%

Caspase-independent death of meiotic and postmeiotic cells overexpressing p53: calpain involvement

et al. 2006

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In a model of male sterility (MTp53) owing to enforced p53 expression in spermatocytes II and spermatids of transgenic mice, we focused on the role of caspases. Most of them are expressed in all differentiation stages, but only the transcriptional levels of caspase-2 and caspase-3 are modified in MTp53 germ cells. In normal testis, cleaved caspase-3 and caspase-9 are detected during the elongation of spermatids. Despite this constitutive presence of caspases during terminal differentiation, calpains are the main effectors of germ cell loss in MTp53 testes: calpain 1 RNA levels are increased, caspase-3-like activity is markedly decreased while calpain activity is higher and the calpain inhibitor E64d ((2S, 3S)-trans-epoxysuccinyl-L-leucylamido-3-methylbutane ethyl ester) reduces TUNEL labeling in MTp53 testis, whereas pancaspase inhibitor zVADfmk (N-benzyloxycarbonyl-ValAla-Asp(OMe)-fluoromethylketone) has no effect. Our work suggests that despite the presence, and potent involvement, of caspases in male haploid cell maturation, calpains are the executioners of the death of terminally differentiating germ cells.

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Activation of Calpain I Converts Excitotoxic Neuron Death into a Caspase-independent Cell Death

Cited by 255 publications

References 55 publications

Multiple death pathways in retina-derived 661W cells following growth factor deprivation: crosstalk between caspases and calpains

Multiple death pathways in retina-derived 661W cells following growth factor deprivation: crosstalk between caspases and calpains

CD44 ligation induces caspase-independent cell death via a novel calpain/AIF pathway in human erythroleukemia cells

Caspase-independent death of meiotic and postmeiotic cells overexpressing p53: calpain involvement

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