Brown-like adipose progenitors derived from human induced pluripotent stem cells: Identification of critical pathways governing their adipogenic capacity

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作者
Anne-Laure Hafner
Julian Contet
Christophe Ravaud
Xi Yao
Phi Villageois
Kran Suknuntha
Karima Annab
Pascal Peraldi
Bernard Binetruy
Igor I. Slukvin
Annie Ladoux
Christian Dani
机构
[1] Université Côte d’Azur,Department of Pathology and Laboratory Medicine
[2] CNRS,undefined
[3] Inserm,undefined
[4] iBV,undefined
[5] Nice,undefined
[6] University of Wisconsin,undefined
[7] Inserm U910,undefined
[8] Faculty of Medicine La Timone,undefined
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Scientific Reports | / 6卷
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摘要
Human induced pluripotent stem cells (hiPSCs) show great promise for obesity treatment as they represent an unlimited source of brown/brite adipose progenitors (BAPs). However, hiPSC-BAPs display a low adipogenic capacity compared to adult-BAPs when maintained in a traditional adipogenic cocktail. The reasons of this feature are unknown and hamper their use both in cell-based therapy and basic research. Here we show that treatment with TGFβ pathway inhibitor SB431542 together with ascorbic acid and EGF were required to promote hiPSCs-BAP differentiation at a level similar to adult-BAP differentiation. hiPSC-BAPs expressed the molecular identity of adult-UCP1 expressing cells (PAX3, CIDEA, DIO2) with both brown (ZIC1) and brite (CD137) adipocyte markers. Altogether, these data highlighted the critical role of TGFβ pathway in switching off hiPSC-brown adipogenesis and revealed novel factors to unlock their differentiation. As hiPSC-BAPs display similarities with adult-BAPs, it opens new opportunities to develop alternative strategies to counteract obesity.
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