高脂肪饮食导致的昼夜节律紊乱会损害血糖控制和骨质量。
Circadian rhythm disruption with high-fat diet impairs glycemic control and bone quality.
机构信息
Department of Biomedical Engineering, Rensselaer Polytechnic Institute, Troy, NY, USA.
Center for Biotechnology and Interdisciplinary Studies, Rensselaer Polytechnic Institute, Troy, NY, USA.
出版信息
FASEB J. 2021 Sep;35(9):e21786. doi: 10.1096/fj.202100610RR.
Biological functions, including glycemic control and bone metabolism, are highly influenced by the body's internal clock. Circadian rhythms are biological rhythms that run with a period close to 24 hours and receive input from environmental stimuli, such as the light/dark cycle. We investigated the effects of circadian rhythm disruption (CRD), through alteration of the light/dark schedule, on glycemic control and bone quality of mice. Ten-week-old male mice (C57/BL6, n = 48) were given a low-fat diet (LFD) or a high-fat diet (HFD) and kept on a dayshift or altered schedule (RSS3) for 22 weeks. Mice were divided into four experimental groups (n = 12/group): Dayshift/LFD, Dayshift/HFD, RSS3/LFD, and RSS3/HFD. CRD in growing mice fed a HFD resulted in a diabetic state, with a 36.2% increase in fasting glucose levels compared to the Dayshift/LFD group. Micro-CT scans of femora revealed a reduction in inner and outer surface expansion for mice on a HFD and altered light schedule. Cancellous bone demonstrated deterioration of bone quality as trabecular number and thickness decreased while trabecular separation increased. While HFD increased cortical bone mineral density, its combination with CRD reduced this phenomenon. The growth of mineral crystals, determined by small angle X-ray scattering, showed HFD led to smaller crystals. Considering modifications of the organic matrix, regardless of diet, CRD exacerbated the accumulation of fluorescent advanced glycation end-products (fAGEs) in collagen. Strength testing of tibiae showed that CRD mitigated the higher strength in the HFD group and increased brittleness indicated by lower post-yield deflection and work-to-fracture. Consistent with accumulation of fAGEs, various measures of toughness were lowered with CRD, but combination of CRD with HFD protected against this decrease. Differences between strength and toughness results represent different contributions of structural and material properties of bone to energy dissipation. Collectively, these results demonstrate that combination of CRD with HFD impairs glycemic control and have complex effects on bone quality.
生物功能,包括血糖控制和骨代谢,受人体内部生物钟的高度影响。昼夜节律是接近 24 小时周期的生物节律,它接收环境刺激的输入,如光/暗周期。我们研究了通过改变光/暗时间表来破坏昼夜节律(CRD)对小鼠血糖控制和骨质量的影响。给予 10 周龄雄性小鼠(C57/BL6,n=48)低脂饮食(LFD)或高脂饮食(HFD),并进行 22 周的日班或改变时间表(RSS3)。将小鼠分为四个实验组(n=12/组):日班/LFD、日班/HFD、RSS3/LFD 和 RSS3/HFD。生长中的 HFD 喂养小鼠的 CRD 导致糖尿病状态,与日班/LFD 组相比,空腹血糖水平增加 36.2%。股骨的 micro-CT 扫描显示,HFD 和改变的光照时间表使小鼠的内表面和外表面扩张减少。松质骨显示骨质量恶化,小梁数量和厚度减少,而小梁分离增加。虽然 HFD 增加了皮质骨骨密度,但与 CRD 结合后,这种现象减少了。通过小角度 X 射线散射确定的矿物质晶体生长表明,HFD 导致晶体变小。考虑到有机基质的修饰,无论饮食如何,CRD 都会加剧胶原蛋白中荧光晚期糖基化终产物(fAGEs)的积累。胫骨强度测试表明,CRD 减轻了 HFD 组的较高强度,并通过较低的屈服后挠度和断裂功来增加脆性。与 fAGEs 的积累一致,CRD 降低了各种韧性测量值,但 CRD 与 HFD 的结合可防止这种降低。强度和韧性结果之间的差异代表了骨的结构和材料特性对能量耗散的不同贡献。总的来说,这些结果表明,CRD 与 HFD 的结合会损害血糖控制,并对骨质量产生复杂影响。
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