Metabolic Regulation of Oocyte Cell Death through the CaMKII-Mediated Phosphorylation of Caspase-2

Nutt, Leta K.; Margolis, Seth S.; Jensen, Mette V.; Herman, Catherine E.; Dunphy, William G.; Rathmell, Jeffrey C.; Kornbluth, Sally

doi:10.1016/j.cell.2005.07.032

Cited by 224 publications

(273 citation statements)

References 52 publications

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“…108 In Xenopus oocytes, CamKIImediated phosphorylation of caspase-2 appears to prevent its activation. 111 These data are consistent with a model that predicts that the main event in caspase-2 activation is precursor dimerisation that is prevented in healthy cells by phosphorylation of caspase-2. Whether this is a general mechanism of caspase-2 activation or limited to specific cell death signalling remains to be determined.…”

Section: The Apoptotic Caspases S Kumarsupporting

confidence: 88%

“…106 Caspase-2 has also been shown to be necessary for TRAIL-mediated, 107,108 heat shock (HS)-induced apoptosis, 109,110 as well as oocyte cell death. 111 Recently, caspase-2 was shown to associate with Fas/CD95 DISC and get activated in that complex, but apparently not required for CD95-induced cell death. 112 Caspase-2 activation occurs rapidly and acute ablation of caspase-2 in a multitude of cell lines inhibits apoptosis in response to a range of stimuli including anticancer drugs.…”

Section: The Apoptotic Caspases S Kumarmentioning

confidence: 99%

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Caspase function in programmed cell death

2006

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The first proapoptotic caspase, CED-3, was cloned from Caenorhabditis elegans in 1993 and shown to be essential for the developmental death of all somatic cells. Following the discovery of CED-3, caspases have been cloned from several vertebrate and invertebrate species. As reviewed in other articles in this issue of Cell Death and Differentiation, many caspases function in nonapoptotic pathways. However, as is clear from the worm studies, the evolutionarily conserved role of caspases is to execute programmed cell death. In this article, I will specifically focus on caspases that function primarily in cell death execution. In particular, the physiological function of caspases in apoptosis is discussed using examples from the worm, fly and mammals.

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Section: The Apoptotic Caspases S Kumarsupporting

confidence: 88%

Section: The Apoptotic Caspases S Kumarmentioning

confidence: 99%

Caspase function in programmed cell death

2006

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“…However, this needs to be directly verified using a catalytically inactive mutant of hexokinase. Other investigators have demonstrated that 2-deoxyglucose-6-phosphate, generated via the action of hexokinase, can be metabolized via the pentose phosphate pathway (PPP) in quantities sufficient to support redox coupling critical for cell survival (Le Goffe et al, 1999Goffe et al, , 2002 and redox coupling between this pathway and caspase-2 activation has also recently been described (Nutt et al, 2005), so potential metabolic contributions distal to glucose phosphorylation cannot be excluded (see below).…”

Section: Mitochondrial Hexokinases As Downstream Effectors Of Growth mentioning

confidence: 99%

“…It was subsequently shown that NADPH leads to the specific inhibition of caspase-2 via phosphorylation of its prodomain. It appears that NADPH activates CaMKII, which phosphorylates a serine residue in the prodomain of caspase-2 and thereby inhibits its activity (Nutt et al, 2005). Whether or not gluconeogenesisderived glucose-6-phosphate can serve a similar role in tissues such as the liver remains to be examined.…”

Section: Gsh Peroxide Inactivationmentioning

confidence: 99%

Mitochondrial hexokinases, novel mediators of the antiapoptotic effects of growth factors and Akt

2006

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Cell survival has been closely linked to both trophic growth factor signaling and cellular metabolism. Such couplings have obvious physiologic and pathophysiologic implications, but their underlying molecular bases remain incompletely defined. As a common mediator of both the metabolic and anti-apoptotic effects of growth factors, the serine/threonine kinase Akt -also known as protein kinase B or PKB -is capable of regulating and coordinating these inter-related processes. The glucose dependence of the antiapoptotic effects of growth factors and Akt plus a strong correlation between Akt-regulated mitochondrial hexokinase association and apoptotic susceptibility suggest a major role for hexokinases in these effects. Mitochondrial hexokinases catalyse the first obligatory step of glucose metabolism and directly couple extramitochondrial glycolysis to intramitochondrial oxidative phosphorylation, and are thus well suited to play this role. The ability of Akt to regulate energy metabolism appears to have evolutionarily preceded the capacity to control cell survival. This suggests that Akt-dependent metabolic regulatory functions may have given rise to glucose-dependent antiapoptotic effects that evolved as an adaptive sensing system involving hexokinases and serve to ensure mitochondrial homeostasis, thereby coupling metabolism to cell survival. We hypothesize that the enlistment of Akt and hexokinase in the control of mammalian cell apoptosis evolved as a response to the recruitment of mitochondria to the apoptotic cascade. The central importance of mitochondrial hexokinases in cell survival also suggests that they may represent viable therapeutic targets in cancer.

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“…45 Caspase-2 is also actively imported into the nucleus via a nuclear localization sequence (NLS) located in the prodomain. 7,8 Caspase-2 activation has been shown to be regulated by phosphorylation mediated by various kinases, including calcium/calmodulin-dependent protein kinase II (Ser164), 47 protein kinase CK2 (Ser157) 48 and cyclin-dependent kinase 1 (Ser340). 49 …”

Section: Caspase-2 -The Anti-cancer Connectionmentioning

confidence: 99%

Caspase-2 as a tumour suppressor

2013

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Ever since its discovery 20 years ago, caspase-2 has been enigmatic and its function somewhat controversial. Although many in vitro studies suggested that caspase-2 was important for apoptosis, demonstrating an in vivo cell death role for this caspase has been more problematic, with caspase-2-deficient mice showing limited, tissue-specific cell death defects. Recent results from different laboratories suggest that at least one of its physiological roles in animals is to protect against cellular stress and transformation. As such, loss of caspase-2 augments tumorigenesis in some mouse models of cancer, assigning a tumour suppressor function to this enigmatic caspase. This review focuses on this seemingly non-apoptotic function of caspase-2 as a tumour suppressor and reconciles some of the recent findings in the field.

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Metabolic Regulation of Oocyte Cell Death through the CaMKII-Mediated Phosphorylation of Caspase-2

Cited by 224 publications

References 52 publications

Caspase function in programmed cell death

Caspase function in programmed cell death

Mitochondrial hexokinases, novel mediators of the antiapoptotic effects of growth factors and Akt

Caspase-2 as a tumour suppressor

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