Neurosteroid modulation of the presynaptic NMDA receptors regulating hippocampal noradrenaline release in normal rats and those exposed prenatally to diazepam

6533b82bfe1ef96bd128e0e7

RESEARCH PRODUCT

Neurosteroid modulation of the presynaptic NMDA receptors regulating hippocampal noradrenaline release in normal rats and those exposed prenatally to diazepam

Debora Altobelli Monia D'amico Maria Martire Carla Cannizzaro Paolo Preziosi

subject

Male Pregnenolone sulfate medicine.medical_specialty Receptor complex Neuroactive steroid Allosteric modulator Glycine Pharmacology Hippocampus Receptors N-Methyl-D-Aspartate Norepinephrine Cellular and Molecular Neuroscience chemistry.chemical_compound Pregnancy Internal medicine Neurosteroid medicine pregnenolone sulphate Animals Rats Wistar Receptor Diazepam GABAA receptor Hippocampal synaptosomes Cell Biology Rats Endocrinology NMDA/GLY-mediated [3H]NA release chemistry Pregnenolone Prenatal Exposure Delayed Effects Settore BIO/14 - Farmacologia NMDA receptor Female Pregnenolone sulfate Synaptosomes Hormone

description

Abstract Prenatal exposure to diazepam (DZ), a positive allosteric modulator of the γ-aminobutyric acidA (GABAA) receptor complex, exerts profound effects that become more evident during puberty and in many cases are sex-specific, suggesting that such exposure interferes with the activity of steroid hormones. Apart from their well known effects on the genome, the reduced metabolites of many steroid hormones also interact directly with membrane receptors, including those for N-methyl- d -aspartate (NMDA). In this study, we compared the effects of several neurosteroids on NMDA receptors from normal rats and those exposed in utero to DZ (1.25 mg/kg per day) from the 14th through the 20th day of gestation. In superfused rat hippocampal synaptosomes, activation of the NMDA receptor stimulates the basal release of [ 3 H ]noradrenaline ([ 3 H ]NA), which was used in our study as an index of receptor function. [ 3 H ]NA release was evoked in a concentration-dependent manner by NMDA (100 μM) plus glycine (GLY). The maximal increase (68.23±3.86%) with respect to basal release was achieved with a GLY concentration of 10 μM, and the EC50 for GLY was 0.1 μM. Release stimulated by 100 μM NMDA+0.1 μM GLY was not modified by any of the neurosteroids tested, with the exception of pregnenolone sulfate (PREG-S), which produced a 78.57±3.94% reduction in release at the maximal concentration used (0.3 μM). In synaptosomes from animals exposed in utero to DZ, the inhibitory effect of PREG-S was reduced by 46.55±2.33%. Given the important roles played by NMDA receptors in physiological and pathological processes within the central nervous system (CNS), characterization of NMDA receptor modulation is an important objective. The fact that this modulation can be altered by exposure in utero to DZ indicates that the behavioral abnormalities observed in exposed animals might be partially attributed to an altered sensitivity of NMDA receptors to the modulatory effects of neurosteroids.

year	journal	country	edition	language
2003-01-01	Neurochemistry International

https://doi.org/10.1016/s0197-0186(02)00226-7