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n-3 多不饱和脂肪酸重塑原代人 CD4+ T 细胞质膜有序性。

Remodelling of primary human CD4+ T cell plasma membrane order by n-3 PUFA.

机构信息

1Program in Integrative Nutrition and Complex Diseases,Departments of Nutrition & Food Science,Texas A&M University,College Station, TX 77843,USA.

4Immunobiology & Transplant Science Center,Houston Methodist,Houston,TX 77030,USA.

出版信息

Br J Nutr. 2018 Jan;119(2):163-175. doi: 10.1017/S0007114517003385. Epub 2017 Dec 18.

Abstract

Cell membrane fatty acids influence fundamental properties of the plasma membrane, including membrane fluidity, protein functionality, and lipid raft signalling. Evidence suggests that dietary n-3 PUFA may target the plasma membrane of immune cells by altering plasma membrane lipid dynamics, thereby regulating the attenuation of immune cell activation and suppression of inflammation. As lipid-based immunotherapy might be a promising new clinical strategy for the treatment of inflammatory disorders, we conducted in vitro and in vivo experiments to examine the effects of n-3 PUFA on CD4+ T cell membrane order, mitochondrial bioenergetics and lymphoproliferation. n-3 PUFA were incorporated into human primary CD4+ T cells phospholipids in vitro in a dose-dependent manner, resulting in a reduction in whole cell membrane order, oxidative phosphorylation and proliferation. At higher doses, n-3 PUFA induced unique phase separation in T cell-derived giant plasma membrane vesicles. Similarly, in a short-term human pilot study, supplementation of fish oil (4 g n-3 PUFA/d) for 6 weeks in healthy subjects significantly elevated EPA (20 : 5n-3) levels in CD4+ T cell membrane phospholipids, and reduced membrane lipid order. These results demonstrate that the dynamic reshaping of human CD4+ T cell plasma membrane organisation by n-3 PUFA may modulate down-stream clonal expansion.

摘要

细胞膜脂肪酸会影响质膜的基本特性,包括膜流动性、蛋白质功能和脂筏信号转导。有证据表明,膳食 n-3PUFA 可能通过改变质膜脂质动力学来靶向免疫细胞的质膜,从而调节免疫细胞激活的衰减和炎症的抑制。由于基于脂质的免疫疗法可能是治疗炎症性疾病的一种有前途的新临床策略,我们进行了体外和体内实验,以研究 n-3PUFA 对 CD4+T 细胞膜有序性、线粒体生物能学和淋巴增殖的影响。n-3PUFA 以剂量依赖性方式掺入人原代 CD4+T 细胞的磷脂中,导致整个细胞膜有序性、氧化磷酸化和增殖减少。在更高的剂量下,n-3PUFA 会在 T 细胞衍生的巨大质膜囊泡中诱导独特的相分离。同样,在一项短期的人体初步研究中,健康受试者补充鱼油(4 克 n-3PUFA/天)6 周,可显著提高 CD4+T 细胞膜磷脂中的 EPA(20:5n-3)水平,并降低膜脂质有序性。这些结果表明,n-3PUFA 对人类 CD4+T 细胞质膜组织的动态重塑可能会调节下游克隆扩增。

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