Early life exposure to clonazepam has both short- and long-term effects on seizures induced with pentylenetetrazol (PTZ)
Hana Kubova, Grygoriy Tsenov, Anita Conti, Alessandro Negri, Lenka Roubalova, Pavel Mares

TL;DR
Early exposure to clonazepam in rats increases seizure risk both shortly and long-term after treatment stops.
Contribution
This study reveals long-term seizure susceptibility changes from early-life clonazepam exposure in rats.
Findings
Early CZP exposure increases generalized tonic-clonic seizure severity for one week after treatment cessation.
CZP exposure reduces latency to absence-like seizures in adult rats but not in juveniles.
Early-life GABAergic inhibition changes permanently alter seizure susceptibility in adulthood.
Abstract
The abrupt cessation of chronic benzodiazepine administration is associated with the development of withdrawal symptoms like increased susceptibility to seizures or seizure development in both animals and humans. Although withdrawal phenomena have been studied in detail in adult animals, information about their development and nature in the immature brain is lacking. Substantial experimental evidence suggests that exposure to BZDs early in life permanently alters brain circuitry and functions. However, the possible long-term modification of seizure propensity has not yet been studied. Clonazepam (CZP) was injected into rat pups daily at a dose of 1 mg/kg for five consecutive days, starting on postnatal day 7 (P7) and continuing until P11. Seizure susceptibility was assessed using a pentylenetetrazol (PTZ)-induced seizure model. PTZ induces three types of seizures in rodents that differ…
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Taxonomy
TopicsNeuroscience and Neuropharmacology Research · Epilepsy research and treatment · Pharmacological Effects and Toxicity Studies
