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Low calcium-phosphate intakes modulate the low-protein diet-related effect on peak bone mass acquisition: A hormonal and bone strength determinants study in female growing rats

机译:磷酸钙摄入不足可调节低蛋白饮食对峰值骨量获取的影响:雌性成年大鼠的激素和骨强度决定因素研究

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摘要

Peak bone mass acquisition is influenced by environmental factors including dietary intake. A low-protein diet delays body and skeletal growth in association with a reduction in serum IGF-1 whereas serum FGF21 is increased by selective amino acid deprivation. Calcium (Ca) and phosphorous (P) are also key nutrients for skeletal health, and inadequate intakes reduce bone mass accrual in association with calciotropic hormone modulation. Besides, the effect of calcium supplementation on bone mass in prepubertal children appears to be influenced by protein intake. To further explore the interaction of dietary protein and Ca-P intake on bone growth, 1-month-old femalerats were fed with an isocaloric 10%, 7.5%, or 5%casein diet containing normal or low Ca-P for an 8-week period (6 groups). Changes in tibia geometry, mineral content, microarchitecture, strength, and intrinsic bone quality were analyzed. At the hormonal level, serum IGF-1, fibroblast growth factor 21 (FGF21), PTH, 1,25-dihydroxyvitamin D3 (calcitriol), and FGF23 were investigated as well as the Ghr hepatic gene expression. In normal dietary Ca-P conditions, bone mineral content, trabecular and cortical bone volume, and bone strength were lower in the 5% casein group in association with a decrease in serum IGF-1 and an increase in FGF21 levels. Unexpectedly, the low-Ca-P diet attenuated the 5% casein diet-related reduction of serum IGF-1 and Ghr hepatic gene expression, as well as the low-protein diet-induced decrease in bone mass and strength. However, this was associated with lower cortical bone material level properties. The low-Ca-P diet increased serum calcitriol but decreased FGF23 levels. Calcitriol levels positively correlated with Ghr hepatic mRNA levels. These results suggest that hormonal modulation in response to a low-Ca-P diet may modify the low-protein diet-induced effect on Ghr hepatic mRNA levels and consequently the impact of low protein intakes on IGF-1 circulating levels and skeletal growth.
机译:峰值骨量获取受环境因素(包括饮食摄入)的影响。低蛋白饮食会延迟人体和骨骼的生长,同时降低血清IGF-1的含量,而血清FGF21则通过选择性氨基酸剥夺而增加。钙(Ca)和磷(P)也是骨骼健康的关键营养素,摄入不足会降低钙质激素调节与骨质积聚的关系。此外,补充钙对青春期前儿童骨量的影响似乎受蛋白质摄入的影响。为了进一步探讨饮食蛋白和Ca-P摄入量对骨骼生长的相互作用,对1个月大的雌性大鼠饲喂了等热量的10%,7.5%或5%酪蛋白饮食,其中含有正常或低Ca-P的8日龄饮食。周期间(6组)。分析了胫骨几何形状,矿物质含量,微结构,强度和固有骨质的变化。在激素水平上,研究了血清IGF-1,成纤维细胞生长因子21(FGF21),PTH,1,25-二羟基维生素D3(骨化三醇)和FGF23以及Ghr肝基因表达。在正常的饮食Ca-P条件下,5%酪蛋白组的骨矿物质含量,小梁和皮质骨量以及骨强度较低,这与血清IGF-1降低和FGF21水平升高有关。出乎意料的是,低钙饮食降低了5%酪蛋白饮食相关的血清IGF-1和Ghr肝基因表达的降低,以及低蛋白质饮食诱导的骨质量和强度的降低。但是,这与较低的皮质骨材料水平特性有关。低钙磷饮食增加血清骨化三醇,但降低FGF23水平。骨化三醇水平与Ghr肝mRNA水平呈正相关。这些结果表明,对低Ca-P饮食的激素调节可能会改变低蛋白质饮食对Ghr肝mRNA水平的影响,从而降低低蛋白质摄入对IGF-1循环水平和骨骼生长的影响。

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