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机械加载对小鼠骨的适应性受昼夜节律影响。

Bone adaptation to mechanical loading in mice is affected by circadian rhythms.

机构信息

Research Centre, Shriners Hospital for Children-Canada, Montreal, Canada; Department of Pediatric Surgery, McGill University, Montreal, Canada; Department of Experimental Surgery, McGill University, Montreal, Canada.

Research Centre, Shriners Hospital for Children-Canada, Montreal, Canada; Department of Pediatric Surgery, McGill University, Montreal, Canada.

出版信息

Bone. 2022 Jan;154:116218. doi: 10.1016/j.bone.2021.116218. Epub 2021 Sep 25.

Abstract

Physical forces are critical for successful function of many organs including bone. Interestingly, the timing of exercise during the day alters physiology and gene expression in many organs due to circadian rhythms. Circadian clocks in tissues, such as bone, express circadian clock genes that target tissue-specific genes, resulting in tissue-specific rhythmic gene expression (clock-controlled genes). We hypothesized that the adaptive response of bone to mechanical loading is regulated by circadian rhythms. First, mice were sham loaded and sacrificed 8 h later, which amounted to tissues being collected at zeitgeber time (ZT)2, 6, 10, 14, 18, and 22. Cortical bone of the tibiae collected from these mice displayed diurnal expression of core clock genes and key osteocyte and osteoblast-related genes, such as the Wnt-signaling inhibitors Sost and Dkk1, indicating these are clock-controlled genes. Serum bone turnover markers did not display rhythmicity. Second, mice underwent a single bout of in vivo loading at either ZT2 or ZT14 and were sacrificed 1, 8, or 24 h after loading. Loading at ZT2 resulted in Sost upregulation, while loading at ZT14 led to Sost and Dkk1 downregulation. Third, mice underwent daily in vivo tibial loading over 2 weeks administered either in the morning, (ZT2, resting phase) or evening (ZT14, active phase). In vivo microCT was performed at days 0, 5, 10, and 15 and conventional histomorphometry was performed at day 15. All outcome measures indicated a robust response to loading, but only microCT-based time-lapse morphometry showed that loading at ZT14 resulted in a greater endocortical bone formation response compared to mice loaded at ZT2. The decreased Sost and Dkk1 expression coincident with the modest, but significant time-of-day specific increase in adaptive bone formation, suggests that circadian clocks influence bone mechanoresponse.

摘要

物理力对于许多器官的正常功能至关重要,包括骨骼。有趣的是,由于昼夜节律,白天运动的时间会改变许多器官的生理和基因表达。组织(如骨骼)中的生物钟表达生物钟基因,这些基因靶向组织特异性基因,导致组织特异性节律性基因表达(时钟控制基因)。我们假设骨骼对机械加载的适应反应受昼夜节律调节。首先,对小鼠进行假加载,然后在 8 小时后处死,相当于在 Zeitgeber 时间(ZT)2、6、10、14、18 和 22 时采集组织。从这些小鼠中采集的胫骨皮质骨显示核心时钟基因和关键成骨细胞和破骨细胞相关基因(如 Wnt 信号抑制剂 Sost 和 Dkk1)的昼夜表达,表明这些是时钟控制基因。血清骨转换标志物没有显示出节律性。其次,将小鼠在 ZT2 或 ZT14 进行单次体内加载,然后在加载后 1、8 或 24 小时处死。在 ZT2 时加载导致 Sost 上调,而在 ZT14 时加载导致 Sost 和 Dkk1 下调。第三,小鼠每天在体内进行胫骨加载,每天在早上(ZT2,休息期)或晚上(ZT14,活动期)进行。在第 0、5、10 和 15 天进行体内 microCT 检查,并在第 15 天进行常规组织形态计量学检查。所有结果指标均表明对加载有强烈反应,但只有基于 microCT 的时间推移形态计量学显示,与在 ZT2 加载的小鼠相比,在 ZT14 加载导致内皮质骨形成反应更大。Sost 和 Dkk1 表达的降低与适应骨形成的适度、但具有时间特异性的增加同时发生,这表明生物钟会影响骨骼的机械反应。

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