Eugenia Marbach-Breitrück scite author profile

Steatosis GLI code? Highlights Hh signaling shows diurnal oscillations in liver and hepatocytes in vitro and in vivo. Hh signaling feeds-back on the liver clock via GLI transcription factors. The amplitude of the oscillations of the liver clock is decreased in hepatocytes from Smo-knockout mice. Rhythmicity of many metabolic pathways, including hepatic lipid metabolism, is affected by oscillating Hh signaling. Diurnal timing of starvation affects the clock-hedgehog module differently.

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Knock-In Mice Expressing a 15-Lipoxygenating Alox5 Mutant Respond Differently to Experimental Inflammation Than Reported Alox5−/− Mice

Marbach-Breitrück

Rohwer

Infante-Duarte

et al. 2021

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Arachidonic acid 5-lipoxygenase (ALOX5) is the key enzyme in the biosynthesis of pro-inflammatory leukotrienes. We recently created knock-in mice (Alox5-KI) which express an arachidonic acid 15-lipoxygenating Alox5 mutant instead of the 5-lipoxygenating wildtype enzyme. These mice were leukotriene deficient but exhibited an elevated linoleic acid oxygenase activity. Here we characterized the polyenoic fatty acid metabolism of these mice in more detail and tested the animals in three different experimental inflammation models. In experimental autoimmune encephalomyelitis (EAE), Alox5-KI mice displayed an earlier disease onset and a significantly higher cumulative incidence rate than wildtype controls but the clinical score kinetics were not significantly different. In dextran sodium sulfate-induced colitis (DSS) and in the chronic constriction nerve injury model (CCI), Alox5-KI mice performed like wildtype controls with similar genetic background. These results were somewhat surprising since in previous loss-of-function studies targeting leukotriene biosynthesis (Alox5−/− mice, inhibitor studies), more severe inflammatory symptoms were observed in the EAE model but the degree of inflammation in DSS colitis was attenuated. Taken together, our data indicate that these mutant Alox5-KI mice respond differently in two models of experimental inflammation than Alox5−/− animals tested previously in similar experimental setups.

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Eugenia Marbach-Breitrück

Tick-tock hedgehog-mutual crosstalk with liver circadian clock promotes liver steatosis

Knock-In Mice Expressing a 15-Lipoxygenating Alox5 Mutant Respond Differently to Experimental Inflammation Than Reported Alox5−/− Mice

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