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人多能脂肪干细胞分化为功能性棕色脂肪细胞。

Human multipotent adipose-derived stem cells differentiate into functional brown adipocytes.

机构信息

IBDC, Université de Nice Sophia-Antipolis, CNRS, 06 107 Nice cedex 2, France.

出版信息

Stem Cells. 2009 Nov;27(11):2753-60. doi: 10.1002/stem.200.

Abstract

In contrast to the earlier contention, adult humans have been shown recently to possess active brown adipose tissue with a potential of being of metabolic significance. Up to now, brown fat precursor cells have not been available for human studies. We have shown previously that human multipotent adipose-derived stem (hMADS) cells exhibit a normal karyotype and high self-renewal ability; they are known to differentiate into cells that exhibit the key properties of human white adipocytes, that is, uncoupling protein two expression, insulin-stimulated glucose uptake, lipolysis in response to beta-agonists and atrial natriuretic peptide, and release of adiponectin and leptin. Herein, we show that, upon chronic exposure to a specific PPARgamma but not to a PPARbeta/delta or a PPARalpha agonist, hMADS cell-derived white adipocytes are able to switch to a brown phenotype by expressing both uncoupling protein one (UCP1) and CIDEA mRNA. This switch is accompanied by an increase in oxygen consumption and uncoupling. The expression of UCP1 protein is associated to stimulation of respiration by beta-AR agonists, including beta3-AR agonist. Thus, hMADS cells represent an invaluable cell model to screen for drugs stimulating the formation and/or the uncoupling capacity of human brown adipocytes that could help to dissipate excess caloric intake of individuals.

摘要

与早期的观点相反,最近的研究表明,成年人确实拥有活跃的棕色脂肪组织,其具有代谢意义的潜力。到目前为止,还没有可供人类研究的棕色脂肪前体细胞。我们之前已经表明,人类多能脂肪源性干细胞(hMADS)表现出正常的核型和高自我更新能力;已知它们可以分化为表现出人类白色脂肪细胞关键特性的细胞,即解偶联蛋白 2 的表达、胰岛素刺激的葡萄糖摄取、β-激动剂和心钠肽诱导的脂肪分解,以及脂联素和瘦素的释放。在此,我们发现,经过慢性暴露于特定的 PPARγ激动剂,而不是 PPARβ/δ或 PPARα激动剂,hMADS 细胞来源的白色脂肪细胞能够通过表达解偶联蛋白 1(UCP1)和 CIDEA mRNA 而转变为棕色表型。这种转变伴随着耗氧量和解偶联的增加。UCP1 蛋白的表达与β-AR 激动剂(包括β3-AR 激动剂)刺激呼吸有关。因此,hMADS 细胞代表了一种非常有价值的细胞模型,可以筛选出刺激人类棕色脂肪细胞形成和/或解偶联能力的药物,这可能有助于消耗个体摄入的多余热量。

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