Inhibition of Caspase-Mediated Apoptosis by Peroxynitrite in Traumatic Brain Injury

Lau, Anthony; Arundine, Mark; Sun, Hong‐Shuo; Jones, Michael W. M.; Tymianski, Michael

doi:10.1523/jneurosci.3507-06.2006

Cited by 68 publications

(54 citation statements)

References 81 publications

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“…Â area (1.49 in 2 ), we calculated that at 2.9 p.s.i., J (on cells) E9.6 N s. We have shown earlier that this sublethal trauma does not confer delayed cell death on its own -as assessed by propidium iodide uptake 20 h after injury -or alter membrane permeability, as assessed by carboxyfluorescein uptake and retention of fluorescein di-acetate. 9 This model is highly consistent with other paradigms of in vitro TBI in the literature, 30,32 which have frequently been used to delineate the intracellular mechanisms that contribute to progressive neuronal injury after mechanical trauma.…”

Section: Methodssupporting

confidence: 66%

“…We used the cells for experiments 11-14 days after isolation consistent with earlier in vitro stretch assays. 24,29,30 In vitro model of mild TBI. Before stretch, the culture medium was replaced with 2 ml HEPES buffered saline (concentrations in mM: 121 NaCl, 5 KCl, 20 glucose, 10 HEPES acid, 7 HEPES-Na salt, 3 NaHCO 3 , 1 Na-pyruvate, 1.8 CaCl 2 and 0.01 glycine, adjusted to pH 7.4 with NaOH).…”

Section: Methodsmentioning

confidence: 99%

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PICK1-mediated GluR2 endocytosis contributes to cellular injury after neuronal trauma

Bell

Park

et al. 2009

Cell Death Differ

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Constitutive and activity-dependent regulation of the AMPA receptor GluR2 content is recognized as an important mediator of both neuronal plasticity and vulnerability to excitotoxic neuron death. In the latter case, inclusion of GluR2 protects against glutamate excitotoxicity in CNS disease by lowering receptor single-channel conductance and preventing deleterious calcium influx. We investigated the hypothesis that aberrations in GluR2 trafficking after in vitro and in vivo cerebral trauma contribute to excitotoxicity and associated calcium-dependent cell death processes. First, in an in vitro model of traumatic brain injury (TBI), we observed PICK1 and N-methyl-D-aspartic acid (NMDA) receptor-dependent phosphorylation and internalization of GluR2. The contributing cell signaling mechanisms involved enhanced binding between PKCa (the kinase that phosphorylates GluR2) and PICK1 (its PDZ-binding partner), and a novel protein interaction between PKCa and the NMDA receptor scaffolding protein PSD-95. Functionally, these phenomena enhanced single cell AMPAR mEPSCs and protracted calcium extrusion. In vivo TBI similarly promoted GluR2 phosphorylation and internalization, with enhanced expression of calcium-permeable AMPARs in the injured hippocampus. Peptide-mediated perturbation of the PKCa/PICK1 protein interaction after trauma preserved surface GluR2 expression, attenuated AMPAR-mediated toxicity, and occluded the sensitivity of neuronal physiology to calcium-permeable AMPAR antagonists. These findings suggest that experimental TBI promotes the expression of injurious GluR2-lacking AMPARs, thereby enhancing cellular vulnerability to secondary excitotoxicity. Traumatic brain injury (TBI) continues to be a leading cause of morbidity and disability in North America. 1 At the cellular level, excitotoxic stimulation of N-methyl-D-aspartate (NMDA) and a-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid (AMPA) glutamatergic receptors has a major function in the deregulation of calcium homeostasis and acute cell swelling after TBI, ultimately leading to secondary neuronal cell death hours to days after the primary injury. 1 Unfortunately, global antagonism of these ionotropic channels (which has generally targeted the highly calciumpermeable NMDARs) is a clinically impractical approach because of interference with physiological receptor function. 2 As such, it remains of critical importance to identify novel potential intracellular targets of anti-excitotoxic therapy to mitigate delayed secondary cell loss, and improve functional outcome after TBI.Physiologically, AMPA receptors mediate the majority of excitatory ionotropic neurotransmission in the CNS. 3 Pathologically, however, AMPA receptors can also mediate excitotoxic neuronal damage when GluR2 subunits are absent from the tetrameric receptor complex 4 (composed of four subunits, GluR1-4). This is because receptors devoid of the GluR2 subunit (e.g. homomers of GluR1) exhibit two-to three-fold increases in single-channel conductance, increased calcium and zinc permeab...

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Section: Methodssupporting

confidence: 66%

Section: Methodsmentioning

confidence: 99%

PICK1-mediated GluR2 endocytosis contributes to cellular injury after neuronal trauma

Bell

Park

et al. 2009

Cell Death Differ

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“…Consistent with this hypothesis, it has been shown that ROS can inhibit calpain activity via oxidation of the sulfhydryl groups of cysteine residues at the active site of the enzyme (Benuck et al, 1992) (Guttmann et al, 1997) (Guttmann and Johnson, 1998). Recent work by another group has shown that another cysteine protease caspase-3 in the traumatized brain is similarly inhibited by PN specifically, and that this is prevented by application of the sulfhydryl reducing agent dithiothreitol (Lau et al, 2006). The latter is also relevant since the SBDP150 fragment which also showed a biphasic time course is partially generated by caspase 3 as well as calpain (Wang, 2000b).…”

Section: Interaction Of Peroxynitrite-induced Oxidative and Calpain-mmentioning

confidence: 79%

Temporal relationship of peroxynitrite-induced oxidative damage, calpain-mediated cytoskeletal degradation and neurodegeneration after traumatic brain injury

Deng

Thompson

Gao

et al. 2007

Experimental Neurology

133

173

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We assessed the temporal and spatial characteristics of PN-induced oxidative damage and its relationship to calpain-mediated cytoskeletal degradation and neurodegeneration in a severe unilateral controlled cortical impact (CCI) traumatic brain injury (TBI) model. Quantitative temporal time-course studies were performed to measure two oxidative damage markers: 3-nitrotyrosine (3NT) and 4-hydroxynonenal (4HNE) at 30 min, 1, 3, 6, 12, 24, 48, 72 hrs, 7 days after injury in ipsilateral cortex of young adult male CF-1 mice. Secondly, the time course of Ca ++ -activated, calpain-mediated proteolysis was also analyzed using quantitative western-blot measurement of breakdown products of the cytoskeletal protein α-spectrin. Finally, the time course of neurodegeneration was examined using de Olmos silver staining. Both oxidative damage markers increased in cortical tissue immediately after injury (30 min) and elevated for the first 3-6 hrs before returning to baseline. In the immunostaining study, the PN-selective marker, 3NT, and the lipid peroxidation marker, 4HNE, were intense and overlapping in the injured cortical tissue. α-Spectrin breakdown products, which was used as biomarker for calpain-mediated cytoskeletal degradation, were also increased after injury, but the time course lagged behind the peak of oxidative damage and did not reach its maximum until 24 hrs post-injury. In turn, cytoskeletal degradation preceded the peak of neurodegeneration which occurred at 48 hrs post-injury. These studies have led us to the hypothesis that PN-mediated oxidative damage is an early event that contributes to a compromise of Ca ++ homeostatic mechanisms which causes a massive Ca ++ overload and calpain activation which is a final common pathway that results in post-traumatic neurodegeneration.

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“…Alternatively, it might be that upregulation of caspases activation in HIBM cells does not result in a concordant upregulation of PS externalization, although this apoptotic phenomenon is known to be caspase dependent. 26 Interestingly, there is accumulating data pointing to caspaseindependent PS externalization occurring during apoptosis, for example in STS-treated primary T lymphocytes, 27 possibly indicating that in some conditions those two processes may be independently activated. Therefore, it may well be that caspases activation, but not PS externalization, is involved in HIBM pathology.…”

Section: Discussionmentioning

confidence: 99%

Characterization of hereditary inclusion body myopathy myoblasts: possible primary impairment of apoptotic events

et al. 2007

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Hereditary inclusion body myopathy (HIBM) is a unique muscular disorder caused by mutations in the UDP-N-acetylglucosamine 2-epimerase/N-acetylmannosamine kinase (GNE) gene. GNE encodes a bi-functional enzyme acting in the biosynthetic pathway of sialic acid. Since the underlying myopathological mechanism leading to the disease phenotype is poorly understood, we have established human myoblasts cultures, derived from HIBM satellite cells carrying the homozygous M712T mutation, and identified cellular and molecular characteristics of these cells. HIBM and control myoblasts showed similar heterogeneous patterns of proliferation and differentiation. Upon apoptosis induction, phosphatidylserine externalization was similar in HIBM and controls. In contrast, the active forms of caspase-3 and -9 were strongly enhanced in most HIBM cultures compared to controls, while pAkt, downregulated in controls, remained high in HIBM cells. These results could indicate impaired apoptotic signaling in HIBM cells. Since satellite cells enable partial regeneration of the post-mitotic muscle tissue, these altered processes could contribute to the muscle mass loss seen in patients. The identification of survival defects in HIBM affected muscle cells could disclose new functions for GNE in muscle cells.

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Inhibition of Caspase-Mediated Apoptosis by Peroxynitrite in Traumatic Brain Injury

Cited by 68 publications

References 81 publications

PICK1-mediated GluR2 endocytosis contributes to cellular injury after neuronal trauma

PICK1-mediated GluR2 endocytosis contributes to cellular injury after neuronal trauma

Temporal relationship of peroxynitrite-induced oxidative damage, calpain-mediated cytoskeletal degradation and neurodegeneration after traumatic brain injury

Characterization of hereditary inclusion body myopathy myoblasts: possible primary impairment of apoptotic events

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