Tumor necrosis factor-α: presynaptic sensitivity is modified after antidepressant drug administration

Presynaptic adrenergic functioning was coupled to cytokine sensitivity in order to further establish the mechanism of action of a tricyclic antidepressant drug. Antidepressant administration of desipramine to rats twice-daily for 2 weeks increased hippocampal TNF levels and transformed the presynapt...

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Veröffentlicht in:Brain research 1994-12, Vol.665 (2), p.293-299
Hauptverfasser: Ignatowski, Tracey A., Spengler, Robert N.
Format: Artikel
Sprache:eng
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Zusammenfassung:Presynaptic adrenergic functioning was coupled to cytokine sensitivity in order to further establish the mechanism of action of a tricyclic antidepressant drug. Antidepressant administration of desipramine to rats twice-daily for 2 weeks increased hippocampal TNF levels and transformed the presynaptic TNF response. One day of desipramine administration resulted in increased locus coeruleus TNF mRNA accumulation and, simultaneously, hippocampal TNF levels escalated. The fractional release of [ 3H]norepinephrine during field stimulation of control hippocampal slices was decreased by the addition of TNF in a concentration-dependent manner, an effect which was potentiated by the α 2-adrenergic antagonist idazoxan. While no change in sensitivity to TNF was observed in the hippocampus after one day of desipramine administration, TNF enhanced, rather than inhibited [ 3H]norepinephrine release after 14 days. In addition, TNF potentiation of [ 3H]norepinephrine release after chronic desipramine administration was reversed in the presence of idazoxan to a greater inhibition than in control slices exposed to idazoxan. Therefore, TNF-induced regulation of [ 3H]norepinephrine releaase appears to be associated with an alteration of α 2-adrenergic receptor responsiveness. The reversal in presynaptic TNF responsiveness after 14 days of tricyclic antidepressant drug administration describes a mechanism of action for their delayed clinical effect.
ISSN:0006-8993
1872-6240
DOI:10.1016/0006-8993(94)91350-1