Attenuation
of the effect of progesterone and 4-chlordiazepam on
stress-induced immune responses by bicuculline
P. K. Mediratta*, J. Bhatia, S.
Tewary, V. Katyal,
P. Mahajan and K. K. Sharma
Department of Pharmacology,
University College of Medical Sciences & GTB Hospital,
Delhi 110 095
( Received on May 1, 2002 )
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Abstract
The present study investigates
the effect of progesterone, a pregnane precursor of neurosteroids,
and 4-chlordiazepam (4'-CD), a specific ligand for mitochondrial
diazepam binding inhibitor receptor (MDR) involved in neurosteroidogenesis,
on restraint stress (RS)-induced modulation of humoral and
cell-mediated immune responses. RS produced a significant
reduction in anti-sheep red blood cells (SRBC) antibody titre,
a measure of humoral immune response, and % leucocyte migration
inhibition (LMI) and foot-pad thickness test, measures of
cell-mediated immune responses. These effects of RS on immune
responses were effectively blocked by pretreating the animals
with progesterone (10 mg/kg, sc) or 4'-CD (0.5 mg/kg, sc)
administered just before subjecting the animal to RS. The
effect of both progesterone and 4'-CD on RS-induced immune
modulation was significantly attenuated by bicuculline (2
mg/kg, ip) but not by flumazenil (10 mg/kg, ip). Unlike its
effect on RS-induced immune responsiveness, progesterone (5,
10 mg/kg, sc) when administered to non-stressed animals produced
a significant suppression of both humoral and cell-mediated
immune responses which was not reversed by bicuculline. However,
4'-CD failed to modulate immune response in naïve non-stressed
animals. These results suggest that progesterone and 4'-CD
affect stress-induced immune responses by modulating GABA-ergic
mechanism. However, GABA-A receptor system does not appear
to be involved in progesterone-induced immunosuppression in
nonstressed animals.