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Participation of a GABA-ergic system in the processes of neuroimmunomodulation.

作者信息

Devoino L, Idova G, Beletskaya I

机构信息

Institute of Physiology Siberian Branch, Academy of Medical Sciences, USSR, Novosibirsk.

出版信息

Int J Neurosci. 1992 Nov-Dec;67(1-4):215-27. doi: 10.3109/00207459208994786.

DOI:10.3109/00207459208994786
PMID:1339052
Abstract

Participation of a GABA-ergic system in neuroimmunomodulation was established through the use of a large number of chemical compounds which selectively modulate the activity of the GABA-BD-receptor-ionophore complex. Activation of the GABA-receptors with muscimol or activation of the BD-receptors with diazepam or tazepam had stimulatory effects upon immunogenesis. A decrease in the GABA-BD-receptor-ionophore complex activity led to a suppression of the immune response. The effect was achieved with: a blockade of the complex with bicuculline--a competitive inhibitor of the GABA-receptors: administration of a specific antagonist of the BD-receptors flumazenil or Ro 15-3505: or with blockade of chloride channels with picrotoxin. Activation of the GABA-ergic system causes an increase in bone marrow content of T-helper cells marked by L3T4. The immunomodulatory action of the GABA-ergic system is of central origin and can occur only when the hypothalamo-pituitary system is intact. Section of the pituitary stalk prevents accumulation of the T-helper cells in the bone marrow. The result show that the influence of GABA-ergic system on immunogenesis requires participation of both dopaminergic and serotoninergic systems.

摘要

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