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长时间久坐期间主动休息对皮下脂肪组织基因表达的急性影响:一项随机对照试验的辅助分析。

Acute effects of active breaks during prolonged sitting on subcutaneous adipose tissue gene expression: an ancillary analysis of a randomised controlled trial.

机构信息

Baker Heart & Diabetes Institute, Melbourne, Australia.

Murdoch Children's Research Institute, and Department of Paediatrics, University of Melbourne, Parkville, VIC, Australia.

出版信息

Sci Rep. 2019 Mar 7;9(1):3847. doi: 10.1038/s41598-019-40490-0.

Abstract

Active breaks in prolonged sitting has beneficial impacts on cardiometabolic risk biomarkers. The molecular mechanisms include regulation of skeletal muscle gene and protein expression controlling metabolic, inflammatory and cell development pathways. An active communication network exists between adipose and muscle tissue, but the effect of active breaks in prolonged sitting on adipose tissue have not been investigated. This study characterized the acute transcriptional events induced in adipose tissue by regular active breaks during prolonged sitting. We studied 8 overweight/obese adults participating in an acute randomized three-intervention crossover trial. Interventions were performed in the postprandial state and included: (i) prolonged uninterrupted sitting; or prolonged sitting interrupted with 2-minute bouts of (ii) light- or (iii) moderate-intensity treadmill walking every 20 minutes. Subcutaneous adipose tissue biopsies were obtained after each condition. Microarrays identified 36 differentially expressed genes between the three conditions (fold change ≥0.5 in either direction; p < 0.05). Pathway analysis indicated that breaking up of prolonged sitting led to differential regulation of adipose tissue metabolic networks and inflammatory pathways, increased insulin signaling, modulation of adipocyte cell cycle, and facilitated cross-talk between adipose tissue and other organs. This study provides preliminary insight into the adipose tissue regulatory systems that may contribute to the physiological effects of interrupting prolonged sitting.

摘要

在长时间久坐中进行主动休息对心血管代谢风险生物标志物有有益影响。其分子机制包括调节控制代谢、炎症和细胞发育途径的骨骼肌基因和蛋白质表达。脂肪组织和肌肉组织之间存在活跃的通讯网络,但主动休息对脂肪组织的影响尚未得到研究。本研究旨在描述在长时间久坐中定期进行主动休息对脂肪组织产生的急性转录事件。我们研究了 8 名超重/肥胖成年人,他们参与了一项急性随机三干预交叉试验。干预措施在餐后进行,包括:(i)长时间不间断的坐姿;或每隔 20 分钟用 2 分钟的(ii)低强度或(iii)中强度跑步机步行打断长时间坐姿。在每种情况下,我们都会从皮下脂肪组织活检中获取样本。微阵列鉴定了三种条件之间的 36 个差异表达基因(变化倍数≥0.5;p<0.05)。途径分析表明,打破长时间坐姿会导致脂肪组织代谢网络和炎症途径的差异调节,增加胰岛素信号,调节脂肪细胞周期,并促进脂肪组织与其他器官之间的交流。这项研究初步揭示了可能有助于中断长时间坐姿的生理效应的脂肪组织调节系统。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/74e5/6405989/adc42564c8d8/41598_2019_40490_Fig1_HTML.jpg

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