Lobular architecture of human adipose tissue defines the niche and fate of progenitor cells

0301 basic medicine 2. Zero hunger Adipogenesis Science Stem Cells Q Subcutaneous Fat Cell Differentiation Nerve Tissue Proteins Receptors, Nerve Growth Factor Intra-Abdominal Fat Alkaline Phosphatase Article Extracellular Matrix [SDV] Life Sciences [q-bio] Transforming Growth Factor beta1 03 medical and health sciences Adipose Tissue Adipocytes Humans Obesity Stem Cell Niche Myofibroblasts
DOI: 10.1038/s41467-019-09992-3 Publication Date: 2019-06-11T10:02:53Z
ABSTRACT
AbstractHuman adipose tissue (hAT) is constituted of structural units termed lobules, the organization of which remains to be defined. Here we report that lobules are composed of two extracellular matrix compartments, i.e., septa and stroma, delineating niches of CD45−/CD34+/CD31− progenitor subsets characterized by MSCA1 (ALPL) and CD271 (NGFR) expression. MSCA1+ adipogenic subset is enriched in stroma while septa contains mainly MSCA1−/CD271− and MSCA1−/CD271high progenitors. CD271 marks myofibroblast precursors and NGF ligand activation is a molecular relay of TGFβ-induced myofibroblast conversion. In human subcutaneous (SC) and visceral (VS) AT, the progenitor subset repartition is different, modulated by obesity and in favor of adipocyte and myofibroblast fate, respectively. Lobules exhibit depot-specific architecture with marked fibrous septa containing mesothelial-like progenitor cells in VSAT. Thus, the human AT lobule organization in specific progenitor subset domains defines the fat depot intrinsic capacity to remodel and may contribute to obesity-associated cardiometabolic risks.
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