Prolonged Therapeutic Window for Ischemic Brain Damage Caused by Delayed Caspase Activation

Fink, Klaus; Zhu, Jinmin; Namura, Shobu; Shimizu‐Sasamata, Masao; Endres, Matthias; Ma, Jiechao; Dalkara, Turgay; Yuan, Junying; Moskowitz, Michael A.

doi:10.1097/00004647-199810000-00003

Cited by 196 publications

(106 citation statements)

References 30 publications

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“…Caspase-3 is also the most abundant cysteine aspartase expressed in adult rodent brain and caspase-3-like enzyme activity and activated caspase-3 subunits are detected in ischemic tissues by immunoblotting and immunohistochemistry (6,7). Treatment with peptide-based caspase inhibitors protects brain from mild ischemic injury and improves neurological deficits (8)(9)(10). We extend the findings above by studying ischemic mechanisms in caspase-3 Ϫ/Ϫ brain in vivo and in vitro.…”

supporting

confidence: 52%

Caspase activation and neuroprotection in caspase-3- deficient mice after in vivo cerebral ischemia and in vitro oxygen glucose deprivation

Huang

et al. 2002

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

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285

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Caspase-3 is a major cell death effector protease in the adult and neonatal nervous system. We found a greater number and higher density of cells in the cortex of caspase-3 ؊/؊ adult mice, consistent with a defect in developmental cell death. Caspase-3 ؊/؊ mice were also more resistant to ischemic stress both in vivo and in vitro. After 2 h of ischemia and 48 h of reperfusion, cortical infarct volume was reduced by 55%, and the density of terminal deoxynucleotidyltransferase-mediated dUTP nick end labeling-positive cells was decreased by 36% compared with wild type. When subjected to oxygen-glucose deprivation (2 h), cortical neurons cultured from mice deficient in caspase-3 expression were also more resistant to cell death by 59%. Mutant brains showed caspase-specific poly-(ADP-ribose) polymerase cleavage product (85-kDa fragment) in vivo and in vitro, suggesting redundant mechanisms and persistence of caspase-mediated cell death. In the present study, we found that caspase-8 mediated poly(ADP-ribose) polymerase cleavage in caspase-3 ؊/؊ neurons in vivo and in vitro. In addition, mutant neurons showed no evidence of compensatory activation by caspase-6 or caspase-7 after ischemia. Taken together, these data extend the pharmacological evidence supporting an important role for caspase-3 and caspase-8 as cell death mediators in mammalian cortex and indicate the potential advantages of targeting more than a single caspase family member to treat ischemic cell injury.

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supporting

confidence: 52%

Caspase activation and neuroprotection in caspase-3- deficient mice after in vivo cerebral ischemia and in vitro oxygen glucose deprivation

Huang

et al. 2002

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

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285

196

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“…31 Moreover, caspase inhibitors are neuroprotective in in vivo and in vitro models of ischemia. [32][33][34][35][36] We have, however, recently found that caspase activation also contributes to endogenous pathway which can protect against ischemic and excitotoxic injury.…”

Section: Caspase Activation In Neuroprotection/ischemic Tolerancementioning

confidence: 99%

The kinder side of killer proteases: Caspase activation contributes to neuroprotection and CNS remodeling

McLaughlin

2004

Apoptosis

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Caspases are a family of cysteine proteases that are expressed as inactive zymogens and undergo proteolytic maturation in a sequential manner in which initiator caspases cleave and activate the effector caspases 3, 6 and 7. Effector caspases cleave structural proteins, signaling molecules, DNA repair enzymes and proteins which inhibit apoptosis. Activation of effector, or executioner, caspases has historically been viewed as a terminal event in the process of programmed cell death. Emerging evidence now suggests a broader role for activated caspases in cellular maturation, differentiation and other non-lethal events. The importance of activated caspases in normal cell development and signaling has recently been extended to the CNS where these proteases have been shown to contribute to axon guidance, synaptic plasticity and neuroprotection. This review will focus on the adaptive roles activated caspases in maintaining viability, the mechanisms by which caspases are held in check so as not produce apoptotic cell death and the ramifications of these observations in the treatment of neurological disorders.

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“…Caspase 3 activation has been detected following focal (and global) ischaemic insults to the brain [14][15][16][17][18][19] where it coincides with areas of enhanced apoptotic cell death 14 and treatment with caspase 3 inhibitors has been reported to reduce infarct size following MCA occlusion. 14,[56][57][58] Moreover, studies in caspase 3-deficient mice indicate that these animals are relatively resistant to ischaemic insults with smaller lesions than their WT littermates.…”

Section: Discussionmentioning

confidence: 99%

“…10 The decreased apoptosis observed in the brain suggested a critical role for caspase 3 in the development of the central nervous system. Caspase 3 has also been implicated in cell death following a number of neurodegenerative insults including global ischaemia, 12,13 focal ischaemia, [14][15][16][17][18][19] transient ischaemia of the spinal cord, 20 neonatal cerebral hypoxia-ischaemia, [21][22][23] traumatic brain injury, [24][25][26] Alzheimer's disease, [27][28][29] Huntington's disease, [30][31][32] and Parkinson's disease. [33][34][35][36][37] It was therefore hypothesized that overexpression of caspase 3 may sensitize the animal to normal (physiological) apoptotic processes that occur during development and natural ageing and confer particular susceptibility to neurodegenerative insults.…”

Section: Introductionmentioning

confidence: 99%

Mice overexpressing human caspase 3 appear phenotypically normal but exhibit increased apoptosis and larger lesion volumes in response to transient focal cerebral ischaemia

et al. 2004

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Caspase 3 activation has been implicated in cell death following a number of neurodegenerative insults. To determine whether caspase genes can affect the susceptibility of cells to neurodegeneration, a transgenic mouse line was created, expressing human caspase 3 under control of its own promoter. The human gene was regulated by the murine homeostatic machinery and human procaspase 3 was expressed in the same tissues as mouse caspase 3. These novel transgenic mice appeared phenotypically and developmentally normal and survived in excess of 2 years. Behavioural assessment using the 5-choice serial reaction time task found no differences from wild-type littermates. Caspase activity was found to be tightly regulated under physiological conditions, however, significantly larger lesions were obtained when transgenic mice were subjected to focal cerebral ischaemia/reperfusion injury compared to wildtype littermates. These data demonstrate that mice overexpressing human caspase 3 are essentially normal, however, they have increased susceptibility to degenerative insults.

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Prolonged Therapeutic Window for Ischemic Brain Damage Caused by Delayed Caspase Activation

Cited by 196 publications

References 30 publications

Caspase activation and neuroprotection in caspase-3- deficient mice after in vivo cerebral ischemia and in vitro oxygen glucose deprivation

Caspase activation and neuroprotection in caspase-3- deficient mice after in vivo cerebral ischemia and in vitro oxygen glucose deprivation

The kinder side of killer proteases: Caspase activation contributes to neuroprotection and CNS remodeling

Mice overexpressing human caspase 3 appear phenotypically normal but exhibit increased apoptosis and larger lesion volumes in response to transient focal cerebral ischaemia

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