PR002118 (Project)

Description:Maternal obesity puts the offspring at high risk of developing obesity and cardio-metabolic diseases in adulthood. Here, using a mouse model of maternal high-fat diet-induced obesity, we show that whole body fat content of the Off-HFD increases significantly from very early age when compared to the Off-RD. We have previously shown significant metabolic and immune perturbations in the bone marrow of newly weaned offspring of obese mothers. Therefore, we hypothesized that lipid metabolism is altered in the bone marrow Off-HFD in newly weaned offspring of obese mothers when compared to the Off-RD. To test this hypothesis, we investigated the lipidomic profile of bone marrow cells collected from three-week-old offspring of regular and high fat diet-fed mothers. Diacylgycerols (DAGs), triacylglycerols (TAGs), sphingolipids and phospholipids, including plasmalogen, and lysophospholipids were remarkably different between the groups, independent of fetal sex. Levels of cholesteryl esters were significantly decreased in offspring of obese mothers, suggesting reduced delivery of cholesterol to bone marrow cells. This was accompanied by age-dependent progression of mitochondrial dysfunction in bone marrow cells. We subsequently isolated CD11b+ myeloid cells from three-week-old mice and conducted metabolomics, lipidomics, and transcriptomics analyses. The lipidomic profiles of these bone marrow myeloid cells were largely similar to that seen in bone marrow cells and included increases in DAGs and phospholipids alongside decreased TAGs, except for long-chain TAGs, which were significantly increased. Our data also revealed significant sex-dependent changes in amino acids and metabolites related to energy metabolism. Transcriptomic analysis revealed altered expression of genes related to major immune pathways including macrophage alternative activation, B-cell receptor signaling, TGF signaling, and communication between the innate and adaptive immune systems. All told, this study revealed lipidomic, metabolomic, and gene expression abnormalities in bone marrow cells broadly, and in bone marrow myeloid cells particularly, in the newly-weaned offspring of obese mothers, which might at least partially explain the progression of metabolic and cardiovascular diseases in their adulthood.
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A subject produced as part of the PR002118 project

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A biosample from Metabolomics produced as part of the PR002118 project

Biosample

A biosample from Metabolomics produced as part of the PR002118 project

Biosample

A biosample from Metabolomics produced as part of the PR002118 project

Biosample

A biosample from Metabolomics produced as part of the PR002118 project

Biosample

A biosample from Metabolomics produced as part of the PR002118 project

Biosample

A biosample from Metabolomics produced as part of the PR002118 project

Biosample

A biosample from Metabolomics produced as part of the PR002118 project

Biosample

A biosample from Metabolomics produced as part of the PR002118 project

File

A 8.70 MB file from Metabolomics produced from OBI:0003097 as part of the PR002118 project

  • Subject

    A subject produced as part of the PR002118 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR002118 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR002118 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR002118 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR002118 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR002118 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR002118 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR002118 project


  • Biosample

    A biosample from Metabolomics produced as part of the PR002118 project


  • File

    A 8.70 MB file from Metabolomics produced from OBI:0003097 as part of the PR002118 project

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