Lipopolysaccharide (LPS)
is a part of gram-negative bacteria recognized by TLR4. Excessive
activation of immune system by LPS induces sepsis. Earlier studies
have shown that exposure to initial small doses of LPS renders the
host more resilient (more tolerant) to subsequent exposure to higher
doses of LPS. This effect is called LPS tolerance (a process more akin to biochemical adaptation).
The new study (1) published
in Nature suggests that aryl hydrocarbon receptor activity controls
LPS tolerance. AhR is host molecule that recognize endogenous
products of tryptophan catabolism called kynurenines. Tryptophan
catabolism in mammals is mediated by enzymes IDO1, IDO2 and TDO2 (this latter enzyme is mainly expressed in liver cells).
The authors examined the
effect of primary LPS challenge on wild type, AhR-KO, IDO1-KO,
IDO2-KO and TDO2-KO mice. Upon exposure to 10mg/kg of LPS, AhR-KO and
TDO2-KO mice showed significantly higher level of mortality compared
to wild-type or IDO2-KO mice. Of note, in these experiments, IDO2-KO mice behaved similar to wild-type mice (it appears that IDO2 plays no meaningful function in vivo) This increase in LPS sensitivity of
AhR-KO and TDO2-KO mice was
still observed when different doses of LPS was used (8-fold and 4-fold increase respectively). Interestingly,
unlike at 2h post-exposure, levels of pro-inflammatory cytokines,
IL-6, TNF-alpha and IL-1beta were higher in AhR-KO and TDO2-KO mice
at 24h post-exposure compared to levels in wild-type mice. An opposite effect was
seen with IL-10. AhR-KO and TDO2-KO mice expressed less IL-10 at 24h
post LPS exposure.
These results indicated
that activity of AhR or production of kynurenines had protective
effect on host after primary LPS challenge. Indeed, LPS challenge of
wild-type mice treated with TDO2 inhibitor dramatically reduced their
survival that was reversed by exogenously administered L-kynurenine.
This therapeutic effect of L-kynurenine was abolished in AhR-KO mice.
To examine the role of
AhR in LPS tolerance, the authors re-exposed wild-type, IDO1-KO,
IDO2-KO mice previously primed with primary dose of LPS. In this
setting, only wild-type and IDO2-KO mice survived secondary LPS
exposure, while IDO1-KO mice all died by day 10 post secondary LPS
exposure. This resilience of wild-type mice to re-exposure to LPS was
mediated by AhR activity since its blockade by specific inhibitor cut
survival rate of pre-exposed wild-type mice. The authors showed
that beneficial effect of AhR was mediated through TGF-beta and
reduced expression of IL-6, TNF-alpha, not seen in IDO1-KO mice.
Finally, to see the
effect of LPS tolerance in clinically relevant infection model, the authors
infected mice with either gram-negative (S. Typhimurium) or gram-positive bacteria (group B Streptococcus).
When mice were pre-exposed to LPS prior to infection with bacteria,
they showed less immunopathology, reduced pro-inflammatory cytokine
production and improved survival in response to infection compared to
untreated control mice.
In summary, this study
confirmed that the products of tryptophan catabolism activates AhR
and contribute to increased tissue tolerance (biochemical adaptation) to secondary exposure to
infection or noxious products.
David
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