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新型基于 18 碳 n-3 脂肪酸的全胃肠外营养用脂肪乳剂在与标准脂肪乳剂的比较中可诱导出更优的免疫代谢表型。

Novel lipid emulsion for total parenteral nutrition based on 18-carbon n-3 fatty acids elicits a superior immunometabolic phenotype in a murine model compared with standard lipid emulsions.

机构信息

Department of Anesthesiology and Pain Medicine and Cardiovascular Research Centre, University of Alberta, Edmonton, Canada.

Department of Pharmacology, University of Alberta, Edmonton, Canada.

出版信息

Am J Clin Nutr. 2022 Dec 19;116(6):1805-1819. doi: 10.1093/ajcn/nqac272.

Abstract

BACKGROUND

While lipid emulsions in modern formulations for total parenteral nutrition (TPN) provide essential fatty acids and dense calories, they also promote inflammation and immunometabolic disruptions.

OBJECTIVES

We aimed to develop a novel lipid emulsion for TPN use with superior immunometabolic actions compared with available standard lipid emulsions.

METHODS

A novel lipid emulsion [Vegaven (VV)] containing 30% of 18-carbon n-3 fatty acids (α-linolenic acid and stearidonic acid) was developed for TPN (VV-TPN) and compared with TPN containing soybean oil-based lipid emulsion (IL-TPN) and fish-oil-based lipid emulsion (OV-TPN). In vivo studies were performed in instrumented male C57BL/6 mice subjected to 7-d TPN prior to analysis of cytokines, indices of whole-body and hepatic glucose metabolism, immune cells, lipid mediators, and mucosal bowel microbiome.

RESULTS

IL-6 to IL-10 ratios were significantly lower in liver and skeletal muscle of VV-TPN mice when compared with IL-TPN or OV-TPN mice. VV-TPN and OV-TPN each increased hepatic insulin receptor abundance and resulted in similar HOMA-IR values, whereas only VV-TPN increased hepatic insulin receptor substrate 2 and maintained normal hepatic glycogen content, effects that were IL-10-dependent and mediated by glucokinase activation. The percentages of IFN-γ- and IL-17-expressing CD4+ T cells were increased in livers of VV-TPN mice, and liver macrophages exhibited primed phenotypes when compared with IL-TPN. This immunomodulation was associated with successful elimination of the microinvasive bacterium Akkermansia muciniphila from the bowel mucosa by VV-TPN as opposed to standard lipid emulsions. Assay of hepatic lipid mediators revealed a distinct profile with VV-TPN, including increases in 9(S)-hydroxy-octadecatrienoic acid. When co-administered with IL-TPN, hydroxy-octadecatrienoic acids mimicked the VV-TPN immunometabolic phenotype.

CONCLUSIONS

We here report the unique anti-inflammatory, insulin-sensitizing, and immunity-enhancing properties of a newly developed lipid emulsion designed for TPN use based on 18-carbon n-3 fatty acids.

摘要

背景

尽管现代全肠外营养(TPN)配方中的脂肪乳剂提供了必需脂肪酸和密集的热量,但它们也促进了炎症和免疫代谢紊乱。

目的

我们旨在开发一种新型的 TPN 用脂肪乳剂,与现有的标准脂肪乳剂相比,具有更好的免疫代谢作用。

方法

开发了一种新型的脂肪乳剂[Vegaven(VV)],其中含有 30%的 18 碳 n-3 脂肪酸(α-亚麻酸和 stearidonic 酸),用于 TPN(VV-TPN),并与含有大豆油的脂肪乳剂(IL-TPN)和含鱼油的脂肪乳剂(OV-TPN)进行了比较。在接受 7 天 TPN 预处理的仪器化雄性 C57BL/6 小鼠中进行了体内研究,分析了细胞因子、全身和肝葡萄糖代谢指数、免疫细胞、脂质介质和肠道微生物群。

结果

与 IL-TPN 或 OV-TPN 小鼠相比,VV-TPN 小鼠肝和骨骼肌中的 IL-6 与 IL-10 比值显著降低。VV-TPN 和 OV-TPN 均增加了肝胰岛素受体丰度,并导致相似的 HOMA-IR 值,而只有 VV-TPN 增加了肝胰岛素受体底物 2 并维持正常的肝糖原含量,这些作用依赖于 IL-10,并通过葡萄糖激酶的激活介导。VV-TPN 小鼠肝脏中 IFN-γ 和 IL-17 表达的 CD4+T 细胞的百分比增加,与 IL-TPN 相比,肝巨噬细胞表现出激活的表型。这种免疫调节与 VV-TPN 成功地从肠道黏膜中消除了微侵袭细菌 Akkermansia muciniphila 有关,而标准的脂肪乳剂则没有。对肝脂质介质的测定显示了 VV-TPN 的独特特征,包括 9(S)-羟基十八碳三烯酸的增加。当与 IL-TPN 共同给药时,羟基十八碳三烯酸模拟了 VV-TPN 的免疫代谢表型。

结论

我们在此报告了一种新开发的基于 18 碳 n-3 脂肪酸的 TPN 用脂肪乳剂的独特的抗炎、胰岛素敏化和增强免疫特性。

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