Li. Romero et al., BACTERIAL LIPOPOLYSACCHARIDE INDUCTION OF IL-6 IN RAT TELENCEPHALIC CELLS IS MEDIATED IN PART BY IL-1, Neuroendocrinology, 57(5), 1993, pp. 892-897
Interleukin-6 (IL-6) appears in the cerebrospinal fluid (CSF) of patie
nts with acute infection of the central nervous system, and in the bra
ins and CSF of experimental animals following systemic or intracerebra
l injection of bacterial endotoxin (Eschericia coli lipopolysaccharide
, LPS). Since LPS is known to induce secretion of interleukin-1 (IL-1)
in many cell types including those of the brain, and IL-1 can induce
IL-6 in brain tissue it appeared reasonable to postulate that the effe
cts of LPS on IL-6 production were mediated through IL-1 induction. To
test this hypothesis, the effects of IL-1 receptor antagonist (IL-1 R
a) on LPS and IL-1-induced IL-6 secretion were tested in a mixed brain
cell culture from 17-day fetal rat, after 12-14 days in culture. IL-6
secretion was induced by IL-1beta in a concentration as low as 1 x 10
(-10) M (p = 0.0008); addition of IL-1 Ra was shown to inhibit IL-1-in
duced changes by 8 7% (p = 0.00 12) at a molar ratio of 100: 1, and by
100% at a molar ratio of 1,000:1. LPS stimulated IL-6 secretion progr
essively over the concentration of 1-100 ng/ml (p = 0.0001). LPS 10 ng
/ml-induced IL-6 secretion was inhibited by 66% by IL-1 Ra in a concen
tration of 1,000 ng/ml (p = 0.0077). The inhibitory effect of IL-1 Ra
was not significantly greater even when used at a concentration of 5,0
00 ng/ml. These findings indicate that LPS-induced IL-6 secretion is m
ediated at least in part through the induction of IL-1. These findings
extend to brain cells the previously reported effects of the antagoni
st on IL-1 responses in immunocompetent cells, and confirm the presenc
e of functional IL-1 receptors in the central nervous system. Since IL
-1 Ra has been shown to be induced by bacterial toxins, and is present
in brain, it is likely that central responses to inflammation (as wel
l as peripheral responses) are regulated by paracrine interaction betw
een IL-1 and IL-1 Ra.