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Critical illness evokes elevated circulating bile acids related to altered hepatic transporter and nuclear receptor expression

95

Citations

24

References

2011

Year

Abstract

Failure to inhibit BA synthesis, up-regulate canalicular BA export, and localize pivotal NR in the hepatocytic nuclei may indicate dysfunctional feedback regulation by increased BA levels. Alternatively, critical illness may result in maintained BA synthesis (CYP7A1), reversal of normal BA transport (BSEP/MRP3), and inhibition of the BA sensor (FXR/RXRα) to increase serum BA levels.

References

YearCitations

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