PR001715 (Project)

Description:Kupffer cells (KCs) are tissue-resident macrophages which colonize the developing liver early during embryogenesis. Throughout development and adulthood, KCs have distinct core functions that are essential for liver and organismal homeostasis, such as supporting fetal erythropoiesis as well as postnatal erythrocyte recycling and liver metabolism. KCs acquire their tissue-specific transcriptional signature immediately after colonizing the liver, mature together with the tissue, and adapt to the tissue’s function. However, whether perturbation of macrophage core functions during development may contribute to or cause disease at postnatal stages is poorly understood. Here, we utilize a maternal obesity model to disturb KC functions during gestation. We show that offspring born to obese mothers develop fatty liver disease that is accompanied by a local pro-inflammatory response, a phenotype that is augmented if the offspring is kept on control diet after birth. Further, transcriptional analyses reveal that KCs undergo developmental programming through the maternal high-fat diet, which lasts until adulthood. The offspring’s KC developmental programming is irreversible despite the switch to control diet and leads to increased lipid uptake in hepatocytes mediated via paracrine factors stemming from KCs. The transcriptional programming of KCs and the fatty liver disease phenotype are rescued by genetic depletion of hypoxia-inducible factor alpha (Hif-1alpha) in macrophages during gestation. These results demonstrate that macrophages rely on an undisturbed development to fulfil their core functions and support organ homeostasis during adulthood, and establish developmental programming of KCs as a therapeutic strategy for metabolic disorders, such as fatty liver disease.
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Biosample

A biosample from Metabolomics produced as part of the PR001715 project

Biosample

A biosample from Metabolomics produced as part of the PR001715 project

Biosample

A biosample from Metabolomics produced as part of the PR001715 project

Biosample

A biosample from Metabolomics produced as part of the PR001715 project

Subject

A subject produced as part of the PR001715 project

Biosample

A biosample from Metabolomics produced as part of the PR001715 project

Biosample

A biosample from Metabolomics produced as part of the PR001715 project

Biosample

A biosample from Metabolomics produced as part of the PR001715 project

Biosample

A biosample from Metabolomics produced as part of the PR001715 project

Biosample

A biosample from Metabolomics produced as part of the PR001715 project

  • Biosample

    A biosample from Metabolomics produced as part of the PR001715 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR001715 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR001715 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR001715 project


  • Subject

    A subject produced as part of the PR001715 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR001715 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR001715 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR001715 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR001715 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR001715 project

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