Abstract
Representative modelling of human adipose tissue functions is central to metabolic research. Tridimensional models able to recreate human adipogenesis in a physiological tissue-like context in vitro are still scarce. We describe the engineering of white adipose tissues reconstructed from their cultured adipose-derived stromal precursor cells. We hypothesize that these reconstructed tissues can recapitulate key functions of AT under basal and pro-inflammatory conditions. These tissues, featuring human adipocytes surrounded by stroma, were stable and metabolically active in long-term cultures (at least 11 weeks). Secretion of major adipokines and growth factors by the reconstructed tissues was determined and compared to media conditioned by human native fat explants. Interestingly, the secretory profiles of the reconstructed adipose tissues indicated an abundant production of leptin, PAI-1 and angiopoietin-1 proteins, while higher HGF levels were detected for the human fat explants. We next demonstrated the responsiveness of the tissues to the pro-inflammatory stimulus TNF-α, as reflected by modulation of MCP-1, NGF and HGF secretion, while VEGF and leptin protein expression did not vary. TNF-α exposure induced changes in gene expression for adipocyte metabolism-associated mRNAs such as SLC2A4, FASN and LIPE, as well as for genes implicated in NF-κB activation. Finally, this model was customized to feature adipocytes representative of progressive stages of differentiation, thereby allowing investigations using newly differentiated or more mature adipocytes. In conclusion, we produced tridimensional tissues engineered in vitro that are able to recapitulate key characteristics of subcutaneous white adipose tissue. These tissues are produced from human cells and their neo-synthesized matrix elements without exogenous or synthetic biomaterials. Therefore, they represent unique tools to investigate the effects of pharmacologically active products on human stromal cells, extracellular matrix and differentiated adipocytes, in addition to compounds modulating adipogenesis from precursor cells.
Highlights
Adipose tissue (AT) is a highly active organ that regained particular attention considering its contributions to obesity-related dysfunctions such as insulin resistance and cardiovascular diseases [1,2,3]
Histological cross-sections reveal numerous adipocytes embedded into the cell-derived Extracellular matrix (ECM). The latter is more homogenously distributed within human reconstructed adipose tissues (hrAT) than for native AT (Fig 1D), for which adipocytes are arranged into fat lobules supported by dispersed ECM-rich stroma
In vitro models adequately recapituling key aspects of adipose tissue biology are needed in order to gain novel insights into the functional roles and biological responses of human adipocytes
Summary
Adipose tissue (AT) is a highly active organ that regained particular attention considering its contributions to obesity-related dysfunctions such as insulin resistance and cardiovascular diseases [1,2,3]. White AT (WAT) predominates in humans, with distinct metabolic contributions of the visceral depots compared to the subcutaneous ones, especially under conditions of weight gain and obesity [4, 5]. WAT depots produce a great variety of active mediators that are secreted into the circulation, impacting on many cell types and tissues [8]. AT secreted factors such as leptin, plasminogen activator inhibitor-1 (PAI-1), angiopoietin-1 (Ang-1), vascular endothelial growth factor (VEGF) and hepatocyte growth factor (HGF) can impact vascular networks by acting on endothelial cell proliferation, migration and permeability. Ang-1 and PAI-1 are known for their ability to influence capillary stability and the coordination between the adipogenic and angiogenic processes occurring during AT expansion [11,12,13,14,15,16]
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