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脂肪组织对饮食诱导炎症的特定储存库反应:类视黄醇相关孤儿受体α(RORα)是否参与其中?

Depot-Specific Response of Adipose Tissue to Diet-Induced Inflammation: The Retinoid-Related Orphan Receptor α (RORα) Involved?

作者信息

Kadiri Sarah, Auclair Martine, Capeau Jacqueline, Antoine Bénédicte

机构信息

Sorbonne Universites, UPMC Universite Paris 06, INSERM, CNRS, Centre de Recherces St. Antoine (CRSA), Paris, France.

出版信息

Obesity (Silver Spring). 2017 Nov;25(11):1948-1955. doi: 10.1002/oby.22006. Epub 2017 Sep 20.

Abstract

OBJECTIVE

Epididymal adipose tissue (EAT), a visceral fat depot, is more closely associated with metabolic dysfunction than inguinal adipose tissue (IAT), a subcutaneous depot. This study evaluated whether the nuclear receptor RORα, which controls inflammatory processes, could be implicated.

METHODS

EAT and IAT were compared in a RORα loss-of-function mouse (sg/sg) and in wild-type (WT) littermates, fed a standard diet (SD) or a Western diet (WD), to evaluate the impact of RORα expression on inflammatory status and on insulin sensitivity (IS) of each fat depot according to the diet.

RESULTS

Sg/sg mice fed the SD exhibited a decreased inflammatory status and a higher IS in their fat depots than WT mice. WD-induced obesity had distinct effects on the two fat depots. In WT mice, EAT exhibited increased inflammation and insulin resistance while IAT showed reduced inflammation and improved IS, together with a depot-specific increase of RORα, and its target gene IκBα, in the stroma vascular fraction (SVF). Conversely, in sg/sg mice, WD increased inflammation and lowered IS of IAT but not of EAT.

CONCLUSIONS

These findings suggest an anti-inflammatory role for RORα in response to WD, which occurs at the level of SVF of IAT, thus possibly contributing to the "healthy" expansion of IAT.

摘要

目的

附睾脂肪组织(EAT)作为一种内脏脂肪库,比皮下脂肪库腹股沟脂肪组织(IAT)与代谢功能障碍的关联更为密切。本研究评估了控制炎症过程的核受体RORα是否与之有关。

方法

在喂食标准饮食(SD)或西式饮食(WD)的RORα功能缺失小鼠(sg/sg)及其野生型(WT)同窝小鼠中比较EAT和IAT,以评估RORα表达根据饮食对每个脂肪库的炎症状态和胰岛素敏感性(IS)的影响。

结果

喂食SD的sg/sg小鼠脂肪库中的炎症状态降低,胰岛素敏感性高于WT小鼠。WD诱导的肥胖对两个脂肪库有不同影响。在WT小鼠中,EAT炎症增加且出现胰岛素抵抗,而IAT炎症减少且胰岛素敏感性改善,同时基质血管部分(SVF)中RORα及其靶基因IκBα在脂肪库中特异性增加。相反,在sg/sg小鼠中,WD增加了IAT的炎症并降低了其胰岛素敏感性,但对EAT没有影响。

结论

这些发现表明RORα在对WD的反应中具有抗炎作用,这发生在IAT的SVF水平,从而可能有助于IAT的“健康”扩张。

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