BONE CATABOLISM

骨分解代谢
  • 文章类型: Journal Article
    Abaloparide是甲状旁腺激素相关蛋白(PTHrP1-34)的肽类似物,并于2017年被批准为治疗骨质疏松症的第二种骨合成代谢肽。我们先前表明间歇性阿巴罗帕拉肽与PTH同样有效(1-34)。本研究旨在比较PTH(1-34)和阿巴罗帕拉肽对年轻雌性野生型小鼠骨骼的分解代谢作用。两个月大的C57Bl/6J雌性小鼠连续输注人PTH(1-34)或80μg/kgBW/天的阿巴罗帕拉肽或载体2周。安乐死时,进行DEXA-PIXImus以评估全身的骨矿物质密度(BMD),股骨,胫骨,和椎骨。在血清中测量骨转换标志物水平,采集股骨进行微计算机断层扫描(μCT)分析和组织形态计量学,将胫骨和胫骨分离为皮质和小梁部分进行基因表达分析。我们的结果表明,在所有部位,输注阿帕拉肽导致BMD的降低与输注PTH(1-34)相似。μCT和组织形态计量学分析显示,皮质骨厚度和BMD的降低相似,与体内双重标记和血清P1NP发现的骨形成速率增加引起的骨转换增加有关,如破骨细胞数量和血清交联的C-端肽所示,骨吸收增加。骨小梁在两种治疗中均未显示出重大变化。小梁和皮质骨的成骨细胞基因表达分析表明,输注PTH(1-34)或abaloparatide导致成骨细胞分化和活性基因的相似和不同作用。与间歇和体外治疗一样,输注的PTH(1-34)和阿巴罗帕拉肽对PTHR1/SIK/HDAC4通路的下游基因如Sost和Mmp13的调节相似,但对PTHR1/SIK/CRTC通路的调节不同.一起来看,在相同的剂量下,输注的阿帕拉肽与输注的PTH(1-34)引起相同的高骨转换,在雌性野生型小鼠中具有净吸收。©2023作者。JBMRPlus由WileyPeriodicalsLLC代表美国骨骼和矿物研究学会出版。
    Abaloparatide is a peptide analog of parathyroid hormone-related protein (PTHrP 1-34) and was approved in 2017 as the second osteoanabolic peptide for treating osteoporosis. We previously showed that intermittent abaloparatide is equally as effective as PTH (1-34). This study was designed to compare the catabolic effects of PTH (1-34) and abaloparatide on bone in young female wild-type mice. Two-month-old C57Bl/6J female mice were continuously infused with human PTH (1-34) or abaloparatide at 80 μg/kg BW/day or vehicle for 2 weeks. At euthanasia, DEXA-PIXImus was performed to assess bone mineral density (BMD) in the whole body, femurs, tibiae, and vertebrae. Bone turnover marker levels were measured in sera, femurs were harvested for micro-computer tomography (μCT) analyses and histomorphometry, and tibiae were separated into cortical and trabecular fractions for gene expression analyses. Our results demonstrated that the infusion of abaloparatide resulted in a similar decrease in BMD as infused PTH (1-34) at all sites. μCT and histomorphometry analyses showed similar decreases in cortical bone thickness and BMD associated with an increase in bone turnover from the increased bone formation rate found by in vivo double labeling and serum P1NP and increased bone resorption as shown by osteoclast numbers and serum cross-linked C-telopeptide. Trabecular bone did not show major changes with either treatment. Osteoblastic gene expression analyses of trabecular and cortical bone revealed that infusion of PTH (1-34) or abaloparatide led to similar and different actions in genes of osteoblast differentiation and activity. As with intermittent and in vitro treatment, both infused PTH (1-34) and abaloparatide similarly regulated downstream genes of the PTHR1/SIK/HDAC4 pathway such as Sost and Mmp13 but differed for those of the PTHR1/SIK/CRTC pathway. Taken together, at the same dose, infused abaloparatide causes the same high bone turnover as infused PTH (1-34) with a net resorption in female wild-type mice. © 2023 The Authors. JBMR Plus published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research.
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  • 文章类型: Journal Article
    众所周知,补充肌酸,主要是结合阻力训练,显着增加肌肉质量和性能(主要是力量)的措施。新兴研究还表明,补充肌酸可能对骨骼生物学指标产生有利影响。这些合成代谢适应可能与肌酸影响细胞水合状态有关,高能磷酸盐代谢,生长因子,肌肉蛋白质动力学,和骨骼重塑过程。不断积累的研究还表明,补充肌酸具有抗炎和抗分解代谢特性,这可能有助于为肌肉和骨骼的增加和运动恢复创造有利的环境。补充肌酸具有降低炎症标志物并可能减弱癌性肿瘤生长进展的能力。从肌肉骨骼的角度来看,有证据表明,补充肌酸可减少肌肉蛋白质分解代谢(主要是男性)和骨吸收,同时进行抗阻训练。这篇简短综述的目的是总结目前的文献,研究各种研究人群中补充肌酸的潜在抗炎和抗分解代谢作用。
    It is well established that creatine supplementation, primarily when combined with resistance training, significantly increases measures of muscle mass and performance (primarily strength). Emerging research also indicates that creatine supplementation may have favorable effects on measures of bone biology. These anabolic adaptations may be related to creatine influencing cellular hydration status, high-energy phosphate metabolism, growth factors, muscle protein kinetics, and the bone remodeling process. Accumulating research also suggests that creatine supplementation has anti-inflammatory and anti-catabolic properties, which may help create a favorable environment for muscle and bone accretion and recovery from exercise. Creatine supplementation has the ability to decrease markers of inflammation and possibly attenuate cancerous tumor growth progression. From a musculoskeletal perspective, there is some evidence to show that creatine supplementation reduces measures of muscle protein catabolism (primarily in males) and bone resorption when combined with resistance training. The purpose of this brief review is to summarize the current body of literature examining the potential anti-inflammatory and anti-catabolic effects of creatine supplementation across various research populations.
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