LIGHT/TNFSF14 Affects Adipose Tissue Phenotype

A. Oranger, G. Colaianni, G. Ingravallo, Vincenza Sara Scarcella, M. Faienza, M. Grano, S. Colucci, G. Brunetti
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Abstract

LIGHT/TNFSF14 is linked to several signaling pathways as a crucial member of a larger immunoregulatory network. It is primarily expressed in inflammatory effector cells, and high levels of LIGHT have been reported in obesity. Thus, with the aim of deepening the knowledge of the role of LIGHT on adipose tissue phenotype, we studied wild-type (WT), Tnfsf14−/−, Rag−/− and Rag-/Tnfsf14- (DKO) mice fed a normal diet (ND) or high-fat diet (HFD). Our results show that, although there is no significant weight gain between the mice with different genotypes, it is significant within each of them. We also detected an increase in visceral White Adipose Tissue (vWAT) weight in all mice fed HFD, together with the lowest levels of vWAT weight in Tnfsf14−/− and DKO mice fed ND with respect to the other strain. Inguinal WAT (iWAT) weight is significantly affected by genotype and HFD. The least amount of iWAT was detected in DKO mice fed ND. Histological analysis of vWAT showed that both the genotype and the diet significantly affect the adipocyte area, whereas the number is affected only by the genotype. In iWAT, the genotype and the diet significantly affect mean adipocyte area and number; interestingly, the area with the least adipocyte was detected in DKO mice fed ND, suggesting a potential browning effect due to the simultaneous lack of mature lymphocytes and LIGHT. Consistently, Uncoupling Protein 1 (UCP1) staining of iWAT demonstrated that few positive brown adipocytes appeared in DKO mice. Furthermore, LIGHT deficiency is associated with greater levels of UCP1, highlighting the lack of its expression in Rag−/− mice. Liver examination showed that all mice fed HFD had a steatotic liver, but it was particularly evident for DKO mice. In conclusion, our study demonstrates that the adipose tissue phenotype is affected by LIGHT levels but also much more by mature lymphocytes.
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LIGHT/TNFSF14 影响脂肪组织表型
LIGHT/TNFSF14作为一个更大的免疫调节网络的重要成员,与多个信号通路相关联。它主要在炎症效应细胞中表达,有报道称肥胖症中 LIGHT 含量较高。因此,为了深入了解 LIGHT 对脂肪组织表型的作用,我们研究了以正常饮食(ND)或高脂饮食(HFD)喂养的野生型(WT)、Tnfsf14-/-、Rag-/- 和 Rag-/Tnfsf14- (DKO)小鼠。我们的研究结果表明,虽然不同基因型的小鼠之间体重增加不明显,但每种基因型的小鼠之间体重增加都很明显。我们还发现,在所有喂食高脂饮食的小鼠中,内脏白色脂肪组织(vWAT)的重量都有所增加,而喂食 ND 的 Tnfsf14-/ 和 DKO 小鼠的内脏白色脂肪组织重量与其他品系相比最低。腹股沟脂肪(iWAT)的重量受基因型和高氟日粮的显著影响。喂食 ND 的 DKO 小鼠检测到的 iWAT 量最少。vWAT的组织学分析表明,基因型和饮食都对脂肪细胞的面积有显著影响,而数量只受基因型的影响。在 iWAT 中,基因型和饮食对脂肪细胞的平均面积和数量有明显影响;有趣的是,在喂食 ND 的 DKO 小鼠中发现脂肪细胞最少的区域,这表明由于同时缺乏成熟淋巴细胞和 LIGHT,可能会产生褐变效应。同样,iWAT 的解偶联蛋白 1(UCP1)染色表明,DKO 小鼠体内出现的棕色脂肪细胞阳性率很低。此外,LIGHT 缺乏与 UCP1 水平升高有关,这突显了 Rag-/- 小鼠缺乏 UCP1 的表达。肝脏检查显示,所有喂食高脂饮食的小鼠都有脂肪肝,但 DKO 小鼠的脂肪肝尤为明显。总之,我们的研究表明,脂肪组织表型受 LIGHT 水平的影响,但成熟淋巴细胞对其影响更大。
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