S. K. A. Sedowofia scite author profile

Pregnant C57BL/6J and CBA mice were administered 60 mg/kg phenobarbital intraperitoneally from days 10 to 16 of gestation. On day 18 of pregnancy half of the control and drug-treated mice were killed and the embryonic brains removed for cell cultures. The remaining mice were allowed to have their litter. After cross-fostering the mice were used for behavioural studies. Pups born to drug-treated CBA mice had birth-weights similar to controls, but their weights had fallen behind controls by day 18 after birth. They were slower at attaining mature responses in tests for sensory motor development and became progressively more hyperactive (three times more active at day 18) compared to controls. Drug-exposed C57 pups also had birth weights similar to controls. After cross-fostering, 19% of control and 31% of drug-exposed pups died, but the remaining drug-exposed pups showed no deficits in weight gain. In contrast to drug-treated CBA pups, drug-exposed C57 pups were slightly quicker in attaining mature responses in some tests. There was no difference in activity between them and their controls. In neurochemical analyses, uptake of neurotransmitters by cerebral cultures from CBA showed that uptake of GABA was increased by 5%, choline by 95%, dopamine 120%, serotonin 165% and noradrenaline by 160% in cultures from drug exposed embryos compared to controls. In cerebral cultures from C57, GABA uptake was reduced by 18%, choline 33%, dopamine 35% and noradrenaline by 25%. Only serotonin uptake was increased by 182% compared to controls. Differences between C57 and CBA were also apparent in the uptake of neurotransmitters by neuronal cultures from the mesencephalon.(ABSTRACT TRUNCATED AT 250 WORDS)

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Effects of anticonvulsant drugs on brain cultures from chick embryos: A comparison with cultures from embryos treated in ovo

Sedowofia

Clayton

1985

Teratog Carcinog Mutagen

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The effects of anticonvulsant drugs phenytoin, phenobarbitone, and sodium valproate on neurons and glia from embryonic chicken brain have been tested. These effects have been compared with those produced in neuronal and glial cultures established from embryos that were injected with the drugs in ovo. Choline acetyl transferase activity and accumulation of gamma-aminobutyric acid were measured in neuronal cultures, and carbonic anhydrase and 2,'3'-cyclic nucleotide 3' phosphohydrolase activities were measured in glial cultures. Similarities have been observed in the morphological and biochemical changes brought about by the in vitro and in vivo treatment with the drugs. The use of in vitro cell culture systems for screening drugs for potential behavioural teratogenic effects is discussed.

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The Humoral Blood Pressure (BP) Drive in Thermal Injury 152

et al. 1996

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Induction of retinopathy in newborn rats using a clinically relevant oxygen profile

McColm

Cunningham

Sedowofia

et al. 2000

Early Human Development

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S. K. A. Sedowofia

Long-term effects of aluminium on the fetal mouse brain

Differential effects of prenatal exposure to phenobarbital on the behaviour and neurochemistry of CBA and C57BL/6J mice

Effects of anticonvulsant drugs on brain cultures from chick embryos: A comparison with cultures from embryos treated in ovo

The Humoral Blood Pressure (BP) Drive in Thermal Injury 152

Induction of retinopathy in newborn rats using a clinically relevant oxygen profile

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