Experimental cerebral ischemia in Mongolian gerbils

Robust ischemic preconditioning has been shown in rodent brain, but there are concerns regarding the persistence of neuron protection. This issue was examined in rat hippocampus following 4-vessel occlusion (4-VO) ischemia, using DC shifts characteristic of ischemic depolarization to reproducibly define insult severity. Preconditioning ischemia producing 2 to 3.5 mins depolarization was followed at intervals of 2, 5, or 7 days by test insults of varied duration, after which CA1 counts were obtained at 1, 2, 4, or 12 weeks. Neuron loss in naive animals increased with depolarization time longer than 4 mins regardless of postischemic survival interval. Preconditioning 2, 5, or 7 days before test insults prolonged the injury threshold evaluated at 1 week survival to 15, 9, or 6 mins, respectively, showing robust protection and a rapid decay of the protected state. However, by 2 weeks survival after preconditioning at a 2-day interval, the injury threshold dramatically regressed from 15 to 9 mins. Thereafter protection remained relatively stable through 1 month, but slight progression of neuron injury was evident at 3 months. Inflammatory responses were seen in both naive and preconditioned hippocampi throughout this interval, appropriate to the extent of neuron injury. These studies show distinct components of transient and lasting protection after ischemic preconditioning. Finally, it was found that ischemic depolarization was delayed by approximately 1 min in optimally preconditioned rat hippocampus, in contrast to previous results in the gerbil, identifying one specific mechanism by which insult severity is reduced in this model.

Section: Temporal Factors In Ischemic Injury and Preconditioningcontrasting

confidence: 62%

Protective Preconditioning by Transient Global Ischemia in the Rat: Components of Delayed Injury Progression and Lasting Protection Distinguished by Comparisons of Depolarization Thresholds for Cell Loss at Long Survival Times

Ueda

Nowak²

2005

“…The eosinophilia was detectable as early as 6 h after TBI. Eosinophilic neurons (Ito et al, 1975;Suh et al, 2000a) were evident in the brains of rats that were traumatized while at 36.51C or 391C, but were virtually absent in hypothermic rats (Figures 5 and 6). In the hyperthermic rats, significantly more eosinophilic neurons were detected than in normothermic rats (Figures 5 and 6).…”

Section: Degeneration Of the Hippocampal Neurons After Traumatic Braimentioning

confidence: 99%

Neurotoxic Zinc Translocation into Hippocampal Neurons is Inhibited by Hypothermia and is Aggravated by Hyperthermia after Traumatic Brain Injury in Rats

Suh

Frederickson

Danscher

2006

Hypothermia reduces excitotoxic neuronal damage after seizures, cerebral ischemia and traumatic brain injury (TBI), while hyperthermia exacerbates damage from these insults. Presynaptic release of ionic zinc (Zn 2 þ ), translocation and accumulation of Zn 2 þ ions in postsynaptic neurons are important mechanisms of excitotoxic neuronal injury. We hypothesized that temperature-dependent modulation of excitotoxicity is mediated in part by temperature-dependent changes in the synaptic release and translocation of Zn 2 þ . In the present studies, we used autometallographic (AMG) and fluorescent imaging of N-(6-methoxy-8-quinolyl)-para-toluenesulfonamide (TSQ) staining to quantify the influence of temperature on translocation of Zn 2 þ into hippocampal neurons in adult rats after weight drop-induced TBI. The central finding was that TBI-induced Zn 2 þ translocation is strongly influenced by brain temperature. Vesicular Zn 2 þ release was detected by AMG staining 1 h after TBI. At 301C, hippocampus showed almost no evidence of vesicular Zn 2 þ release from presynaptic terminals; at 36.51C, the hippocampus showed around 20% to 30% presynaptic vesicular Zn 2 þ release; and at 391C vesicular Zn 2 þ release was significantly greater (40% to 60%) than at 36.51C. At 6 h after TBI, intracellular Zn 2 þ accumulation was detected by the TSQ staining method, which showed that Zn 2 þ translocation also paralleled the vesicular Zn 2 þ release. Neuronal injury, assessed by counting eosinophilic neurons, also paralleled the translocation of Zn 2 þ , being minimal at 301C and maximal at 391C. We conclude that pathological Zn 2 þ translocation in brain after TBI is temperature-dependent and that hypothermic neuronal protection might be mediated in part by reduced Zn 2 þ translocation.

“…Key Words: Global ischemia-Apoptosis Necrosis-Delayed neuronal death-In situ end labeling-Rat in their subcellular organelles (Petito and Pulsinelli, 1984a,b), The postischemic interval required for the ap parent development of selective neuronal necrosis is in versely proportional to the severity or duration of the ischemic insult-the so-called maturation phenomena described by Ito et al (Ito et at, 1975), This interval is especially prolonged in the CAl neurons of the hippo campus (Ito et aI., 1975; Pulsinelli et aI, 1982a). The term delayed neuronal death has been applied to this process (Kirino, 1982).…”

mentioning

confidence: 99%

DNA Fragmentation Follows Delayed Neuronal Death in CA1 Neurons Exposed to Transient Global Ischemia in the Rat

Petito

Torres-Muñoz

Roberts

et al. 1997

143

Summary: Apoptosis is an active, gene-directed process of cell death in which early fragmentation of nuclear DNA pre cedes morphological changes in the nucleus and, later, in the cytoplasm, In ischemia, biochemical studies have detected oli gonucleosomes of apoptosis whereas sequential morphological studies show changes consistent with necrosis rather than ap optosis, To resolve this apparent discrepancy, we subjected rats to 10 minutes of transient forebrain ischemia followed by I to 14 days of reperfusion, Parameters evaluated in the CAl region of the hippocampus included morphology, in situ end labeling (ISEL) of fr'l-gmented DNA, and expression of p53, Neurons were indistinguishable from controls at postischemic day I but displayed cytoplasmic basophilia or focal condensations at day 2; some neurons were slightly swollen and a few appearedThe neuronal response to brain ischemia depends on the severity and duration of the ischemic insult as well as on intrinsic neuronal factors that impart selective vulner ability to specific brain regions (Scholz, 1953), Brief periods of global ischemia kill vulnerable neurons in the CAl region of the hippocampus whereas longer intervals of vascular occlusion kill neurons in the cerebral cortex and corpus striatum as well (Ito et aI., 1975; Pulsinelli et aI., 1982a), Although seemingly undamaged, neurons in other brain regions such as the CA3 region of the hip pocampus or the paramedian cerebral cortex undergo transient alterations as evidenced by reversible changes 967normaL In situ end labeling was absent At days 3 and 5, approximately 40 to 60% of CAl neurons had shrunken eosin ophilic cytoplasm and pyknotic nuclei, but only half of these were ISEL By day 14, many of the necrotic neurons had been removed by phagocytes; those remaining retained mild ISEL Neither p53 protein nor mRNA were identified in control or postischemic brain by in situ hybridization with riboprobes or by northern blot analysis, These results show that DNA frag mentation occurs after the development of delayed neuronal death in CA I neurons subjected to 10 minutes of global isch emia, They suggest that mechanisms other than apoptosis may mediate the irreversible changes in the CAl neurons in this model. Key Words: Global ischemia-Apoptosis Necrosis-Delayed neuronal death-In situ end labeling-Rat in their subcellular organelles (Petito and Pulsinelli, 1984a,b), The postischemic interval required for the ap parent development of selective neuronal necrosis is in versely proportional to the severity or duration of the ischemic insult-the so-called maturation phenomena described by Ito et al. (Ito et at, 1975), This interval is especially prolonged in the CAl neurons of the hippo campus (Ito et aI., 1975; Pulsinelli et aI, 1982a). The term delayed neuronal death has been applied to this process (Kirino, 1982).During the past few years, the concept of cell death via apoptosis has become increasingly important. This mechanism of cell death is mediated by regulated path ways involving defined gene product...