Temporal relation of calcium-calmodulin binding and neuronal damage after global ischemia in rats.

DeGraba, Thomas J.; Ostrow, Peter T.; Strong, Roger; Earls, R; Zong, Zhaojing; Grotta, James C.

doi:10.1161/01.str.23.6.876

Cited by 18 publications

(8 citation statements)

References 23 publications

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“…A similar phenomenon was noted after severe global ischemia, although after a much shorter duration of ischemia (10 minutes). 3 The area of infarction measured by hematoxylin and eosin staining correlated very closely with the area of the "'central core" of extensive CaM staining loss after 24 hours of ischemia (Fig 2, A and B). Areas of milder loss of CaM staining (considered border zone areas) did not show up as infarct in comparable slices by hematoxylin and eosin staining after 1 hour of occlusion and 23 hours of reperfusion (Fig 2, C and D).…”

Section: Methodssupporting

confidence: 58%

Threshold of calcium disturbances after focal cerebral ischemia in rats. Implications of the window of therapeutic opportunity.

DeGraba¹,

Ostrow²,

Grotta³

1993

Stroke

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Section: Methodssupporting

confidence: 58%

Threshold of calcium disturbances after focal cerebral ischemia in rats. Implications of the window of therapeutic opportunity.

DeGraba¹,

Ostrow²,

Grotta³

1993

Stroke

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“…The area of each hemisphere was determined by threshold analysis and automated planimetry. 38 Following the method of Cavaleri, the hemisphere volume was calculated by summing the areas of the individual sections and multiplying by the mean distance between adjacent sections. 39 To obtain compartment volumes rapidly, we adapted the stereological method of point counting, after we found planimetry to be inaccurate and time consuming.…”

Section: Methodsmentioning

confidence: 99%

Combination therapy protects ischemic brain in rats. A glutamate antagonist plus a gamma-aminobutyric acid agonist.

Lyden

Lonzo

1994

Stroke

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The excitotoxic effects of glutamate can be blocked almost completely with gamma-aminobutyric acid (GABA), an inhibitory neurotransmitter, in cell culture, tissue slices, and in some animal models. After stroke in rats, we showed previously that an agonist of GABA, muscimol, was as neuroprotective as MK-801, an antagonist of glutamate. To obtain further neuroprotection and to avoid the side effects associated with high doses of MK-801, we wanted to assess the efficacy of the two agents in combination. Treatment was administered 5 minutes after embolic cerebral ischemia in Sprague-Dawley rats. The subjects were rated using a neurological evaluation 48 hours later. Visual-spatial learning was measured 8 to 10 weeks after stroke, after which we measured the volume of each cerebral hemisphere and several large cerebral compartments. Treatment groups included saline (n = 27), MK-801 1.0 mg/kg (n = 23), muscimol 1.0 mg/kg (n = 17), and both agents together using a dose of 0.5 mg/kg each (n = 25). A probit analysis of the neurological ratings revealed a protective effect of muscimol used alone (MK-801 potency ratio, 2.0; P = NS; muscimol potency ratio, 4.0; P < .05) and a protective effect of the combination (potency ratio, 5.0; P < .05). Focal ischemia caused a moderate to severe delay in the acquisition of visual-spatial information, which was completely eliminated by the combination treatment but only partially ameliorated with MK-801 or muscimol alone. Ischemia reduced the cerebral hemisphere volume from 0.42 mm3 to 0.34 mm3 (P < .0001), the volume density of cortex from 22% to 17% of total cerebral volume (P < .01), and that of hippocampus from 4.3% to 3.0% (P < .05). Only the combination was neuroprotective, as measured by the ratio of the lesioned to the contralateral hemisphere volume (P = .013). The combination treatment and MK-801 protected the hemisphere volume, the cortex, and the hippocampus and reduced the size of visible infarction. Combination therapy, using a glutamate antagonist and a GABA-A agonist, appeared to protect the brain and ameliorate a defect in learning behavior after stroke. The combination may have been more effective than either agent used alone, although further study of higher doses is needed.

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“…However, many events that have been described seem to follow in a fairly predictable order. [3][4][5][6] First, there is reduction of blood flow followed rapidly by inhibition of protein synthesis, depletion of intracellular energy stores, membrane depolarization, and release of intracellular potassium. This is accompanied by an initial increase in oxygen extraction and glucose metabolism and lactic acidosis.…”

Section: Ischemic Cascadementioning

confidence: 99%

Neuroprotective Therapy

Hickenbottom¹,

Grotta²

1998

Semin Neurol

103

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The concept of neuroprotection relies on the principle that delayed neuronal injury occurs after ischemia. The phenomenon of the "ischemic cascade" has been described, and each step along this cascade provides a target for therapeutic intervention. In animal models of global and focal cerebral ischemia, numerous preclinical studies have demonstrated various agents to be neuroprotective at different steps along this cascade. A wide variety of drugs has also been studied in humans. Ten classes of neuroprotective agents have reached phase III efficacy trials but have shown mixed results. They include calcium channel antagonists, NMDA receptor antagonists, lubeluzole, CDP-choline, the free radical scavenger tirilizad, anti-intercellular adhesion molecule-1 (ICAM-1) antibody, GM-1 ganglioside, clomethiazole, the sodium channel antagonist fosphenytoin, and piracetam. In the future, clinicians may have an armamentarium of treatments for acute ischemic stroke at their disposal, with a combination of agents directed at different sites in the ischemic cascade being the ultimate goal.

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Temporal relation of calcium-calmodulin binding and neuronal damage after global ischemia in rats.

Cited by 18 publications

References 23 publications

Threshold of calcium disturbances after focal cerebral ischemia in rats. Implications of the window of therapeutic opportunity.

Threshold of calcium disturbances after focal cerebral ischemia in rats. Implications of the window of therapeutic opportunity.

Combination therapy protects ischemic brain in rats. A glutamate antagonist plus a gamma-aminobutyric acid agonist.

Neuroprotective Therapy

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