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Publication : Single-cell RNA transcriptomics in mice reveals embryonic origin of fibrosis due to maternal obesity.

First Author  Hossain MN Year  2024
Journal  EBioMedicine Volume  109
Pages  105421 PubMed ID  39476533
Mgi Jnum  J:358425 Mgi Id  MGI:7781636
Doi  10.1016/j.ebiom.2024.105421 Citation  Hossain MN, et al. (2024) Single-cell RNA transcriptomics in mice reveals embryonic origin of fibrosis due to maternal obesity. EBioMedicine 109:105421
abstractText  BACKGROUND: Over 40% of pregnant women in the USA are obese which negatively affects fetal development and offspring health. Maternal obesity (MO) leads to fibrotic infiltration in multiple tissues and organs of offspring during their adulthood although the origin and mechanisms are unclear. METHODS: C57BL/6J female mice were fed a control and high-fat diet to mimic MO condition. Embryonic somatic tissues were obtained at E9.5, E11.5, and E13.5 (equivalent to 6 weeks of human pregnancy) from control (CON) and MO mice for single-cell RNA-sequencing (scRNA-seq). To explore the role of AMP-activated protein kinase (AMPK), AMPK was activated by metformin and A769662, and knocked out in embryonic mesenchymal cells (EMC) using AMPKalpha1 floxed mice. FINDINGS: Using unsupervised clustering, we identified three major cell populations with fibrogenic capacity. Compared to CON, the population of fibrogenic cells increased dramatically (by approximately 125%) due to MO, supporting an embryonic origin of fibrosis in the offspring. MO induced inflammatory response and elevated expression of transforming growth factor beta (TGFbeta) signalling and fibrogenic genes in embryos. MO inhibited AMPK and its activation by metformin and A769662 inhibited TGFbeta signalling and fibrogenesis. INTERPRETATION: MO profoundly enhances embryonic fibrogenesis, explaining the origin of fibrosis in the offspring of mothers living with obesity. Our data underscore the importance of early intervention, before 5-6 weeks of pregnancy, in improving embryonic development, and AMPK is an amiable target for suppressing excessive fibrogenesis in MO embryos to assist increasing populations of obese mothers having healthy children. FUNDING: This work was funded by National Institutes of Health Grant R01HD067449.
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