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ω-3 脂肪酸与脂肪组织生物学。

Omega-3 fatty acids and adipose tissue biology.

机构信息

Department of Adipose Tissue Biology, Institute of Physiology of the Czech Academy of Sciences, Videnska, 1083 Prague 4, Czech Republic.

Department of Adipose Tissue Biology, Institute of Physiology of the Czech Academy of Sciences, Videnska, 1083 Prague 4, Czech Republic.

出版信息

Mol Aspects Med. 2018 Dec;64:147-160. doi: 10.1016/j.mam.2018.01.004. Epub 2018 Jan 17.

Abstract

This review provides evidence for the importance of white and brown adipose tissue (i.e. WAT and BAT) function for the maintenance of healthy metabolic phenotype and its preservation in response to omega-3 polyunsaturated fatty acids (omega-3 PUFA), namely in the context of diseased states linked to aberrant accumulation of body fat, systemic low-grade inflammation, dyslipidemia and insulin resistance. More specifically, the review deals with (i) the concept of immunometabolism, i.e. how adipose-resident immune cells and adipocytes affect each other and define the immune-metabolic interface; and (ii) the characteristic features of "healthy adipocytes" in WAT, which are relatively small fat cells endowed with a high capacity for mitochondrial oxidative phosphorylation, triacylglycerol/fatty acid (TAG/FA) cycling and de novo lipogenesis (DNL). The intrinsic metabolic features of WAT and their flexible regulations, reflecting the presence of "healthy adipocytes", provide beneficial local and systemic effects, including (i) protection against in situ endoplasmic reticulum stress and related inflammatory response during activation of adipocyte lipolysis; (ii) prevention of ectopic fat accumulation and dyslipidemia caused by increased hepatic VLDL synthesis, as well as prevention of lipotoxic damage of insulin signaling in extra-adipose tissues; and also (iii) increased synthesis of anti-inflammatory and insulin-sensitizing lipid mediators with pro-resolving properties, including the branched fatty acid esters of hydroxy fatty acids (FAHFAs), also depending on the activity of DNL in WAT. The "healthy adipocytes" phenotype can be induced in WAT of obese mice in response to various stimuli including dietary omega-3 PUFA, especially when combined with moderate calorie restriction, and possibly also with other life style (e.g. physical activity) or pharmacological (e.g. thiazolidinediones) interventions. While omega-3 PUFA could exert beneficial systemic effects by improving immunometabolism of WAT without a concomitant induction of BAT, it is currently not clear whether the metabolic effects of the combined intervention using omega-3 PUFA and calorie restriction or thiazolidinediones depend also on the activation of BAT function and/or the induction of brite/beige adipocytes in WAT. It remains to be established why omega-3 PUFA intervention in type 2 diabetic subjects does not improve insulin sensitivity and glucose homeostasis despite inducing various anti-inflammatory mediators in WAT, including the recently discovered docosahexaenoyl esters of hydroxy linoleic acid, the lipokines from the FAHFA family, as well as several endocannabinoid-related anti-inflammatory lipids. To answer the question whether and to which extent omega-3 PUFA supplementation could promote the formation of "healthy adipocytes" in WAT of human subjects, namely in the obese insulin-resistant patients, represents a challenging task that is of great importance for the treatment of some serious non-communicable diseases.

摘要

这篇综述提供了证据,证明白色和棕色脂肪组织(即 WAT 和 BAT)的功能对于维持健康的代谢表型及其在 omega-3 多不饱和脂肪酸(omega-3 PUFA)中的保存很重要,即在与异常体脂积累、全身低度炎症、血脂异常和胰岛素抵抗相关的疾病状态下。更具体地说,该综述涉及(i)免疫代谢的概念,即脂肪组织驻留的免疫细胞和脂肪细胞如何相互影响并定义免疫代谢界面;(ii)WAT 中“健康脂肪细胞”的特征,即相对较小的脂肪细胞具有高线粒体氧化磷酸化、甘油三酯/脂肪酸(TAG/FA)循环和从头脂肪生成(DNL)能力。WAT 的内在代谢特征及其灵活的调节反映了“健康脂肪细胞”的存在,提供了有益的局部和全身效应,包括(i)在脂肪分解激活时防止内质网应激和相关炎症反应;(ii)防止由于肝 VLDL 合成增加引起的异位脂肪积累和血脂异常,以及防止胰岛素信号在脂肪外组织中的脂毒性损伤;(iii)增加具有促解决特性的抗炎和胰岛素增敏脂质介质的合成,包括支链脂肪酸酯的羟基脂肪酸(FAHFAs),也取决于 WAT 中的 DNL 活性。在肥胖小鼠的 WAT 中,可以响应各种刺激诱导“健康脂肪细胞”表型,包括饮食中的 omega-3 PUFA,尤其是与适度热量限制联合使用时,也可能与其他生活方式(如体力活动)或药理学(如噻唑烷二酮)干预联合使用。虽然 omega-3 PUFA 通过改善 WAT 的免疫代谢而不伴随 BAT 的诱导来发挥有益的全身效应,但目前尚不清楚使用 omega-3 PUFA 和热量限制或噻唑烷二酮的联合干预的代谢效应是否也依赖于 BAT 功能的激活和/或 WAT 中 brite/beige 脂肪细胞的诱导。尚不清楚为什么 omega-3 PUFA 干预 2 型糖尿病患者尽管在 WAT 中诱导了各种抗炎介质,包括最近发现的二十二碳六烯酸羟化亚油酸酯、FAHFA 家族的脂类以及几种内源性大麻素相关的抗炎脂质,但不能改善胰岛素敏感性和葡萄糖稳态。要回答 omega-3 PUFA 补充是否以及在何种程度上可以促进人类受试者(即肥胖胰岛素抵抗患者)WAT 中“健康脂肪细胞”的形成的问题,这是一个具有重要意义的挑战,对于某些严重的非传染性疾病的治疗至关重要。

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