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Dynamic control of adipose tissue development and adult tissue homeostasis by platelet-derived growth factor receptor alpha

Sunhye Shin, Yiyu Pang, Jooman Park, Lifeng Liu, Brandon Lukas, Seung Hyeon Kim, Ki-Wook Kim, Pingwen Xu, Daniel C. Berry, Yuwei Jiang

2020eLife65 citationsDOIOpen Access PDF

Abstract

Adipocytes arise from distinct progenitor populations during developmental and adult stages but little is known about how developmental progenitors differ from adult progenitors. Here, we investigate the role of platelet-derived growth factor receptor alpha (PDGFRα) in the divergent regulation of the two different adipose progenitor cells (APCs). Using in vivo adipose lineage tracking and deletion mouse models, we found that developmental PDGFRα+ cells are adipogenic and differentiated into mature adipocytes, and the deletion of Pdgfra in developmental adipose lineage disrupted white adipose tissue (WAT) formation. Interestingly, adult PDGFRα+ cells do not significantly contribute to adult adipogenesis, and deleting Pdgfra in adult adipose lineage did not affect WAT homeostasis. Mechanistically, embryonic APCs require PDGFRα for fate maintenance, and without PDGFRα, they underwent fate change from adipogenic to fibrotic lineage. Collectively, our findings indicate that PDGFRα+ cells and Pdgfra gene itself are differentially required for WAT development and adult WAT homeostasis.

Topics & Concepts

BiologyAdipose tissueAdipogenesisPDGFRAProgenitor cellCell biologyGrowth factorWhite adipose tissuePlatelet-derived growth factorPlatelet-derived growth factor receptorEndocrinologyStem cellInternal medicineCancer researchStromal cellReceptorGeneticsMedicineGiSTAdipose Tissue and MetabolismAdipokines, Inflammation, and Metabolic DiseasesMesenchymal stem cell research