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Time and sex dependent effects of magnesium sulphate on post‐asphyxial seizures in preterm fetal sheep
Author(s) -
Bennet Laura,
Galinsky Robert,
Draghi Vittoria,
Lear Christopher A.,
Davidson Joanne O.,
Unsworth Charles P.,
Gunn Alistair J.
Publication year - 2018
Publication title -
the journal of physiology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.802
H-Index - 240
eISSN - 1469-7793
pISSN - 0022-3751
DOI - 10.1113/jp275627
Subject(s) - fetus , asphyxia , medicine , anesthesia , anticonvulsant , in utero , gestation , epilepsy , saline , perinatal asphyxia , neuroprotection , convulsion , pregnancy , endocrinology , biology , genetics , psychiatry
Key points We evaluated the effect of magnesium sulphate (MgSO 4 ) on seizures induced by asphyxia in preterm fetal sheep. MgSO 4 did not prevent seizures, but significantly reduced the total duration, number of seizures, seizure amplitude and average seizure burden. Saline‐asphyxia male fetuses had significantly more seizures than female fetuses, but male fetuses showed significantly greater reduction in seizures during MgSO 4 infusion than female fetuses. A circadian profile of seizure activity was observed in all fetuses, with peak seizures seen around 04.00–06.00 h on the first and second days after the end of asphyxia. This study is the first to demonstrate that MgSO 4 has utility as an anti‐seizure agent after hypoxia–ischaemia. More information is needed about the mechanisms mediating the effect of MgSO 4 on seizures and sexual dimorphism, and the influence of circadian rhythms on seizure expression.Abstract Seizures are common in newborns after asphyxia at birth and are often refractory to anti‐seizure agents. Magnesium sulphate (MgSO 4 ) has anticonvulsant effects and is increasingly given to women in preterm labour for potential neuroprotection. There is limited information on its effects on perinatal seizures. We examined the hypothesis that MgSO 4 infusion would reduce fetal seizures after asphyxia in utero . Preterm fetal sheep at 0.7 gestation (104 days, term = 147 days) were given intravenous infusions of either saline ( n = 14) or MgSO 4 ( n = 12, 160 mg bolus + 48 mg h −1 infusion over 48 h). Fetuses underwent umbilical cord occlusion (UCO) for 25 min, 24 h after the start of infusion. The start time for seizures did not differ between groups, but MgSO 4 significantly reduced the total number of seizures ( P < 0.001), peak seizure amplitude ( P < 0.05) and seizure burden ( P < 0.005). Within the saline‐asphyxia group, male fetuses had significantly more seizures than females ( P < 0.05). Within the MgSO 4 ‐asphyxia group, although both sexes had fewer seizures than the saline‐asphyxia group, the greatest effect of MgSO 4 was on male fetuses, with reduced numbers of seizures ( P < 0.001) and seizure burden ( P < 0.005). Only 1 out of 6 MgSO 4 males had seizures on the second day post‐UCO compared to 5 out of 6 MgSO 4 female fetuses ( P = 0.08). Finally, seizures showed a circadian profile with peak seizures between 04.00 and 06.00 h on the first and second day post‐UCO. Collectively, these results suggest that MgSO 4 may have utility in treating perinatal seizures and has sexually dimorphic effects.