2010
DOI: 10.3389/fnins.2010.00054
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Pharmacological preconditioning with GYKI 52466: a prophylactic approach to neuroprotection

Abstract: Some toxins and drugs can trigger lasting neuroprotective mechanisms that enable neurons to resist a subsequent severe insult. This “pharmacological preconditioning” has far-reaching implications for conditions in which blood flow to the brain is interrupted. We have previously shown that in vitro preconditioning with the AMPA receptor antagonist GYKI 52466 induces tolerance to kainic acid (KA) toxicity in hippocampus. This effect persists well after washout of the drug and may be mediated via inverse agonism … Show more

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Cited by 16 publications
(12 citation statements)
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“…To verify the noncytotoxic effect of the GYKI-52466 solution, sham-infected mice received the same dose of AMPA receptor antagonist. As described in the literature, this pharmacological dose has been reported to have no behavioral effects and to induce neuroprotective actions (20,40).…”
Section: Infectious-virus Assaysmentioning
confidence: 68%
“…To verify the noncytotoxic effect of the GYKI-52466 solution, sham-infected mice received the same dose of AMPA receptor antagonist. As described in the literature, this pharmacological dose has been reported to have no behavioral effects and to induce neuroprotective actions (20,40).…”
Section: Infectious-virus Assaysmentioning
confidence: 68%
“…KA administration resulted in a rapid induction of hypoactivity followed by WDS behaviours before developing limbic seizures. 21 Clonidine was effective in slowing the onset to seizure behaviours, decreasing cumulative seizure score and WDS behaviours. This was similar to previous reports where clonidine decreased WDS and protected against limbic seizures.…”
Section: Discussionmentioning
confidence: 95%
“…Transmitter implantation and electrode positioning procedures were performed as previously described. 13,21 Animals were housed individually post-surgery and left to recovery for 7 days before seizure induction.…”
Section: Surgical Implantation Of Telemetric Transmittersmentioning
confidence: 99%
“…GYKI 52,466 (10 mg/kg) is another non-competitive AMPAR negative allosteric modulator, which shows effective anti-convulsive effects in a number of epilepsy models. However, GYKI 52,466 debilitates motor and cognitive side effects have been routinely documented at doses over 20 mg/kg [ 33 , 34 ]. Thus, it is likely that AMPAR antagonists may be more effective to inhibit spontaneous seizure activity than NMDAR antagonists.…”
Section: Introductionmentioning
confidence: 99%