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胰岛素样生长因子1通过内源性脂肪干细胞/祖细胞的谱系偏向促进脂肪生成。

IGF1 Promotes Adipogenesis by a Lineage Bias of Endogenous Adipose Stem/Progenitor Cells.

作者信息

Hu Li, Yang Guodong, Hägg Daniel, Sun Guoming, Ahn Jeffrey M, Jiang Nan, Ricupero Christopher L, Wu June, Rodhe Christine Hsu, Ascherman Jeffrey A, Chen Lili, Mao Jeremy J

机构信息

Department of Stomatology, Union Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, Hubei, People's Republic of China.

Center for Craniofacial Regeneration (CCR), New York, New York, USA.

出版信息

Stem Cells. 2015 Aug;33(8):2483-95. doi: 10.1002/stem.2052. Epub 2015 May 27.

Abstract

Adipogenesis is essential for soft tissue reconstruction following trauma or tumor resection. We demonstrate that CD31(-)/34(+)/146(-) cells, a subpopulation of the stromal vascular fraction (SVF) of human adipose tissue, were robustly adipogenic. Insulin growth factor-1 (IGF1) promoted a lineage bias towards CD31(-)/34(+)/146(-) cells at the expense of CD31(-)/34(+)/146(+) cells. IGF1 was microencapsulated in poly(lactic-co-glycolic acid) scaffolds and implanted in the inguinal fat pad of C57Bl6 mice. Control-released IGF1 induced remarkable adipogenesis in vivo by recruiting endogenous cells. In comparison with the CD31(-)/34(+)/146(+) cells, CD31(-)/34(+)/146(-) cells had a weaker Wnt/β-catenin signal. IGF1 attenuated Wnt/β-catenin signaling by activating Axin2/PPARγ pathways in SVF cells, suggesting IGF1 promotes CD31(-)/34(+)/146(-) bias through tuning Wnt signal. PPARγ response element (PPRE) in Axin2 promoter was crucial for Axin2 upregulation, suggesting that PPARγ transcriptionally activates Axin2. Together, these findings illustrate an Axin2/PPARγ axis in adipogenesis that is particularly attributable to a lineage bias towards CD31(-)/34(+)/146(-) cells, with implications in adipose regeneration.

摘要

脂肪生成对于创伤或肿瘤切除后的软组织重建至关重要。我们证明,人脂肪组织基质血管成分(SVF)的一个亚群CD31(-)/34(+)/146(-)细胞具有强大的脂肪生成能力。胰岛素生长因子-1(IGF1)促进了向CD31(-)/34(+)/146(-)细胞的谱系偏向,而以CD31(-)/34(+)/146(+)细胞为代价。IGF1被微囊化在聚乳酸-乙醇酸共聚物支架中,并植入C57Bl6小鼠的腹股沟脂肪垫。对照释放的IGF1通过募集内源性细胞在体内诱导了显著的脂肪生成。与CD31(-)/34(+)/146(+)细胞相比,CD31(-)/34(+)/146(-)细胞的Wnt/β-连环蛋白信号较弱。IGF1通过激活SVF细胞中的Axin2/PPARγ途径减弱Wnt/β-连环蛋白信号传导,表明IGF1通过调节Wnt信号促进CD31(-)/34(+)/146(-)偏向。Axin2启动子中的PPARγ反应元件(PPRE)对于Axin2的上调至关重要,表明PPARγ转录激活Axin2。总之,这些发现阐明了脂肪生成中的Axin2/PPARγ轴,这一轴尤其归因于向CD31(-)/34(+)/146(-)细胞的谱系偏向,对脂肪再生具有重要意义。

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