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遗传变异影响了多样性杂交小鼠群体的八个创始品系后肢去负荷的骨骼反应。

Genetic variation influences the skeletal response to hindlimb unloading in the eight founder strains of the diversity outbred mouse population.

机构信息

Virginia Commonwealth University, Richmond, Virginia, USA.

University of Virginia, Charlottesville, Virginia, USA.

出版信息

J Orthop Res. 2024 Jan;42(1):134-140. doi: 10.1002/jor.25646. Epub 2023 Jun 27.

Abstract

During disuse, mechanical unloading causes extensive bone loss, decreasing bone volume and strength. Variations in bone mass and risk of osteoporosis are influenced by genetics; however, it remains unclear how genetic variation affects the skeletal response to unloading. We previously found that genetic variation affects the musculoskeletal response to 3 weeks of immobilization in the 8 Jackson Laboratory J:DO founder strains: C57Bl/6J, A/J, 129S1/SvImJ, NOD/ShiLtJ, NZO/HlLtJ, CAST/EiJ, PWK/PhJ, and WSB/EiJ. Hindlimb unloading (HLU) is the best model for simulating local and systemic contributors of disuse and therefore may have a greater impact on bones than immobilization. We hypothesized that genetic variation would affect the response to HLU across the eight founder strains. Mice of each founder strain were placed in HLU for 3 weeks, and the femurs and tibias were analyzed. There were significant HLU and mouse strain interactions on body weight, femur trabecular BV/TV, and femur ultimate force. This indicates that unloading only caused significant catabolic effects in some mouse strains. C57BL/6 J mice were most affected by unloading while other strains were more protected. There were significant HLU and mouse strain interactions on gene expression of genes encoding bone metabolism genes in the tibia. This indicates that unloading only caused significant effects on bone metabolism genes in some mouse strains. Different mouse strains respond to HLU differently, and this can be explained by genetic differences. These results suggest the outbred J:DO mice will be a powerful model for examining the effects of genetics on the skeletal response to HLU.

摘要

在不使用期间,机械卸载会导致广泛的骨质流失,减少骨量和骨强度。骨量的变化和骨质疏松症的风险受遗传因素影响;然而,遗传变异如何影响骨骼对卸载的反应仍不清楚。我们之前发现,遗传变异会影响 8 个杰克逊实验室 J:DO 创始品系的 3 周固定的肌肉骨骼反应:C57Bl/6J、A/J、129S1/SvImJ、NOD/ShiLtJ、NZO/HlLtJ、CAST/EiJ、PWK/PhJ 和 WSB/EiJ。下肢卸载(HLU)是模拟废用局部和全身因素的最佳模型,因此可能对骨骼的影响大于固定。我们假设遗传变异会影响 8 个创始品系对 HLU 的反应。每个创始品系的小鼠均被置于 HLU 中 3 周,然后分析股骨和胫骨。体重、股骨小梁 BV/TV 和股骨最大力均存在 HLU 和小鼠品系的显著交互作用。这表明只有在某些小鼠品系中,卸载才会引起明显的分解代谢作用。C57BL/6J 小鼠受卸载影响最大,而其他品系则受到更多保护。胫骨中编码骨代谢基因的基因表达也存在 HLU 和小鼠品系的显著交互作用。这表明只有在某些小鼠品系中,卸载才会对骨代谢基因产生显著影响。不同的小鼠品系对 HLU 的反应不同,这可以用遗传差异来解释。这些结果表明,杂交 J:DO 小鼠将成为研究遗传对 HLU 骨骼反应影响的有力模型。

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