Active caspase‐3 expression during postnatal development of rat cerebellum is not systematically or consistently associated with apoptosis

Oomman, Sowmini; Finckbone, VelvetLee; Dertien, Janet; Attridge, Jennifer; Henne, W.; Medina, Margarita S.; Mansouri, Bobbak; Singh, Hema; Strahlendorf, Howard K.; Strahlendorf, Jean C.

doi:10.1002/cne.20223

Cited by 52 publications

(47 citation statements)

References 48 publications

(59 reference statements)

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“…Although it has been suggested that the presence of cleaved caspase-3 represents a point of no return in the apoptotic pathway (Huppertz et al, 1999), this form of the enzyme has also been identified in cells that are not undergoing apoptosis (Oomman et al, 2004). We found that astrocytes throughout the spinal cord of both SNI and naive rats showed moderate to high levels of cleaved caspase-3, and a similar observation has been made in naive rat spinal cord in two previous studies (Martin and Liu, 2002;Hoang et al, 2003).…”

Section: Detection Of Apoptotic Cells With Antibody Against Cleaved Csupporting

confidence: 86%

Loss of Neurons from Laminas I-III of the Spinal Dorsal Horn Is Not Required for Development of Tactile Allodynia in the Spared Nerve Injury Model of Neuropathic Pain

Polgár¹,

Hughes²,

Arham³

et al. 2005

J. Neurosci.

127

108

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It has been proposed that death of inhibitory interneurons in the dorsal horn contributes to the neuropathic pain that follows partial nerve injury. In this study, we have used two approaches to test whether there is neuronal death in the dorsal horn in the spared nerve injury (SNI) model. We performed a stereological analysis of the packing density of neurons in laminas I-III 4 weeks after operation and found no reduction on the ipsilateral side compared with that seen on the contralateral side or in sham-operated or naive rats. In addition, we used two markers of apoptosis, terminal deoxynucleotidyl transferase-mediated biotinylated UTP nick end labeling (TUNEL) staining and immunocytochemical detection of cleaved (activated) caspase-3. Neither of these methods demonstrated apoptotic neurons in the dorsal spinal cord 1 week after operation. Although TUNEL-positive cells were present throughout the gray and white matter at this stage, they were virtually all labeled with antibody against ionized calcium-binding adapter molecule 1, a marker for microglia. All animals that underwent SNI showed clear signs of tactile allodynia affecting the ipsilateral hindpaw. These results suggest that a significant loss of neurons from the dorsal horn is not necessary for the development of tactile allodynia in the SNI model.

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Section: Detection Of Apoptotic Cells With Antibody Against Cleaved Csupporting

confidence: 86%

Loss of Neurons from Laminas I-III of the Spinal Dorsal Horn Is Not Required for Development of Tactile Allodynia in the Spared Nerve Injury Model of Neuropathic Pain

Polgár¹,

Hughes²,

Arham³

et al. 2005

J. Neurosci.

127

108

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“…Although the preponderance of data has emerged from work in the immune system and peripheral organs, several studies have also suggested non-apoptotic roles of caspase-3 in the CNS. Under physiological conditions, caspase-3 has been implicated in neuronal cytoskeletal changes (Rohn et al, 2004), in synaptic remodeling (Dash et al, 2000;Shimohama et al, 2001), in neuronal survival associated with preconditioning (Garnier et al 2003;McLaughlin et al, 2003;Tanaka et al, 2004), in the differentiation of cerebellar Bergmann glial cells (Oomman et al, 2004(Oomman et al, , 2005(Oomman et al, , 2006, and as a marker of astroglial subpopulations (Noyan-Ashraf et al, 2005). Accordingly, following excitotoxic damage in the neonatal brain we have demonstrated that presence of cleaved caspase-3 in nitrated reactive astrocytes in the absence of cell death (Acarin et al, 2005).…”

Section: Introductionmentioning

confidence: 76%

“…In addition, caspase-3 activation and substrate cleavage has been reported in the absence of cell death in gerbil hypoxia (Garnier et al, 2004) and in ischemic tolerance where neuronal caspase-3 is essential for the neuroprotective effect of preconditioning (Garnier et al 2003;McLaughlin et al, 2003;Tanaka et al, 2004). Furthermore, other studies have also demonstrated a role of caspase-3 in the maturation of cerebellar granular cells during development (Oomman et al, 2004) and the differentiation of neural progenitor cells in the olfactory bulb (Fernando et al, 2005;Yan et al, 2001). Progenitor cells that divide and migrate through the rostral migratory stream en route to the olfactory bulb, show cleaved caspase-3 but no signs of cell death (Yan et al, 2001).…”

Section: Presence Of Caspase-cleaved Gfapmentioning

confidence: 96%

“…With regards to glial cell differentiation, Oomann and coworkers, who have described cleaved caspase-3 in Bergmann glia during postnatal development in the absence of apoptotic or proliferation markers, have demonstrated a role of this protease in differentiation processes (Oomman et al, 2004(Oomman et al, , 2005(Oomman et al, , 2006. In addition, it was recently shown that constitutive non-apoptotic expression of the cleaved form of caspase-3 occurs in the nuclei of a subpopulation of astrocytes in the cerebellar cortex, hippocampus, and spinal cord of adult rats of different strains, which show expression of the sodium dependent glutamate transporter (EAAT1, GLAST) (Noyan-Ashraf et al, 2005).…”

Section: Presence Of Caspase-cleaved Gfapmentioning

confidence: 99%

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Caspase‐3 activation in astrocytes following postnatal excitotoxic damage correlates with cytoskeletal remodeling but not with cell death or proliferation

Acarín¹,

Villapol²,

Faiz³

et al. 2007

Glia

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Caspase-3 has classically been defined as the main executioner of programmed cell death. However, recent data supports the participation of this protease in non-apoptotic cellular events including cell proliferation, cell cycle regulation, and cellular differentiation. In this study, astroglial cleavage of caspase-3 was analyzed following excitotoxic damage in postnatal rats to determine if its presence is associated with apoptotic cell death, cell proliferation, or cytoskeletal remodeling. A well-characterized in vivo model of excitotoxicity was studied, where damage was induced by intracortical injection of N-methyl-D-asparate (NMDA) in postnatal day 9 rats. Our results demonstrate that cleaved caspase-3 was mainly observed in the nucleus of activated astrocytes in the lesioned hemisphere as early as 4 h postlesion and persisted until the glial scar was formed at 7-14 days, and it was not associated with TUNEL labeling. Caspase-3 enzymatic activity was detected at 10 h and 1 day postlesion in astrocytes, and co-localized with caspasecleaved fragments of glial fibrillary acidic protein (CCP-GFAP). However, at longer survival times, when astroglial hypertrophy was observed, astroglial caspase-3 did not generally correlate with GFAP cleavage, but instead was associated with de novo expression of vimentin. Moreover, astroglial caspase-3 cleavage was not associated with BrdU incorporation. These results provide further evidence for a nontraditional role of caspases in cellular function that is independent of cell death and suggest that caspase activation is important for astroglial cytoskeleton remodeling following cellular injury. V V C 2007 Wiley-Liss, Inc.

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“…In the developing mouse forebrain, the expression pattern of CC3 correlates well with terminal deoxynucleotidyl transferase-mediated biotinylated UTP nick end labeling (TUNEL)-positive cells with the majority of CC3 ϩ cells being TUNEL ϩ (Urase et al, 2003). However, there are reports that CC3 staining does not always correlate with apoptosis; yet, in these special cases, the CC3 ϩ cells do not have any other characteristics consistent with apoptosis such as chromosome condensation, DNA fragmentation, or TUNEL staining (Yan et al, 2001;Lossi et al, 2004;Oomman et al, 2004).…”

Section: Increased Apoptosis In the Developing Neuroepithelium Of Shcmentioning

confidence: 99%

Neural-Specific Inactivation of ShcA Results in Increased Embryonic Neural Progenitor Apoptosis and Microencephaly

et al. 2006

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Brain size is precisely regulated during development and involves coordination of neural progenitor cell proliferation, differentiation, and survival. The adapter protein ShcA transmits signals from receptor tyrosine kinases via MAPK (mitogen-activated protein kinase)/ ERK (extracellular signal-regulated kinase) and PI3K (phosphatidylinositol 3-kinase)/Akt signaling pathways. In the CNS, ShcA expression is high during embryonic development but diminishes as cells differentiate and switches to ShcB/Sck/Sli and ShcC/N-Shc/Rai. To directly test ShcA function in brain development, we used Cre/lox technology to express a dominant-negative form of ShcA (ShcFFF) in nestin-expressing neural progenitors. ShcFFF-expressing mice display microencephaly with brain weights reduced to 50% of littermate controls throughout postnatal and adult life. The cerebrum appeared most severely affected, but the gross architecture of the brain is normal. Body weight was mildly affected with a delay in reaching mature weight. At a mechanistic level, the ShcFFF microencephaly phenotype appears to be primarily attributable to elevated apoptosis levels throughout the brain from embryonic day 10.5 (E10.5) to E12, which declined by E14.5. Apoptosis remained at normal basal levels throughout postnatal development. Proliferation indices were not significantly altered in the embryonic neuroepithelium or within the postnatal subventricular zone. In another approach with the same nestin-Cre transgene, conditional deletion of ShcA in mice with a homozygous floxed shc1 locus also showed a similar microencephaly phenotype. Together, these data suggest a critical role for ShcA in neural progenitor survival signaling and in regulating brain size.

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Active caspase‐3 expression during postnatal development of rat cerebellum is not systematically or consistently associated with apoptosis

Cited by 52 publications

References 48 publications

Loss of Neurons from Laminas I-III of the Spinal Dorsal Horn Is Not Required for Development of Tactile Allodynia in the Spared Nerve Injury Model of Neuropathic Pain

Loss of Neurons from Laminas I-III of the Spinal Dorsal Horn Is Not Required for Development of Tactile Allodynia in the Spared Nerve Injury Model of Neuropathic Pain

Caspase‐3 activation in astrocytes following postnatal excitotoxic damage correlates with cytoskeletal remodeling but not with cell death or proliferation

Neural-Specific Inactivation of ShcA Results in Increased Embryonic Neural Progenitor Apoptosis and Microencephaly

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