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n-3 PUFAs enhance the frequency of murine B-cell subsets and restore the impairment of antibody production to a T-independent antigen in obesity

机译:n-3 PUFA增强了肥胖小鼠B细胞亚群的频率并恢复了针对肥胖非T非依赖性抗原的抗体产生的损害

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摘要

The role of n-3 polyunsaturated fatty acids (PUFA) on in vivo B-cell immunity is unknown. We first investigated how n-3 PUFAs impacted in vivo B-cell phenotypes and antibody production in the absence and presence of antigen compared with a control diet. Lean mice consuming n-3 PUFAs for 4 weeks displayed increased percentage and frequency of splenic transitional 1 B cells. Upon stimulation with trinitrophenylated-lipopolysaccharide, n-3 PUFAs increased the number of splenic transitional 1/2, follicular, premarginal, and marginal zone B cells. n-3 PUFAs also increased surface, but not circulating, IgM. We next tested the effects of n-3 PUFAs in a model of obesity that is associated with suppressed humoral immunity. An obesogenic diet after ten weeks of feeding, relative to a lean control, had no effect on the frequency of B cells but lowered circulating IgM upon antigen stimulation. Administration of n-3 PUFAs to lean and obese mice increased the percentage and/or frequency of transitional 1 and marginal zone B cells. Furthermore, n-3 PUFAs in lean and obese mice increased circulating IgM relative to controls. Altogether, the data show n-3 PUFAs enhance B cell-mediated immunity in vivo, which has implications for immunocompromised populations, such as the obese.
机译:n-3多不饱和脂肪酸(PUFA)对体内B细胞免疫的作用尚不清楚。我们首先研究了在没有和存在抗原的情况下,与对照饮食相比,n-3 PUFA如何影响体内B细胞表型和抗体产生。消耗n-3 PUFA 4周的瘦小鼠显示脾脏过渡1 B细胞的百分比和频率增加。在用三硝基苯基化的脂多糖刺激后,n-3 PUFA增加了脾脏过渡性1/2细胞,滤泡细胞,边缘前细胞和边缘区B细胞的数量。 n-3 PUFAs也增加了IgM的表面,但没有增加。接下来,我们在与抑制体液免疫有关的肥胖症模型中测试了n-3 PUFA的作用。相对于瘦肉对照组,喂食十周后的致肥胖饮食对B细胞的频率没有影响,但在抗原刺激后降低了循环IgM。向瘦和肥胖的小鼠施用n-3 PUFA可增加过渡1细胞和边缘B区细胞的百分比和/或频率。此外,相对于对照组,瘦和肥胖小鼠中的n-3 PUFAs增加了循环IgM。总体而言,数据显示n-3 PUFA增强了B细胞介导的体内免疫力,这对免疫功能低下的人群(例如肥胖)有影响。

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