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饮食限制对SENCAR、C57BL/6和DBA/2小鼠全身、股骨和椎骨的影响。

Effects of dietary restriction on total body, femoral, and vertebral bone in SENCAR, C57BL/6, and DBA/2 mice.

作者信息

Brochmann Elsa J, Duarte Maria Eugenia, Zaidi Hasan A, Murray Samuel S

机构信息

Geriatric Research Education and Clinical Center, Veterans Affairs Greater Los Angeles Healthcare System, Sepulveda, CA 91343, USA.

出版信息

Metabolism. 2003 Oct;52(10):1265-73. doi: 10.1016/s0026-0495(03)00194-x.

Abstract

Dietary restriction (DR) increases the life span and retards aging, in part, by limiting free radical generation and oxidative damage. DR also reduces body mass, a major determinant of bone mass across the life span. We tested the hypothesis that DR has its most beneficial effects on bone in mouse strains with high free radical generation (sensitive to carcinogenesis [SENCAR] > C57 > DBA) versus the hypothesis that bone mass at weight-bearing sites is determined by body mass in DR and ad libitum (AL)-fed mice. Male mice of each strain were killed at 10 weeks of age (t(0)) or randomized to an AL-fed or 30% DR feeding regimen for 6 months. Food consumption by AL-fed mice was measured daily, and DR mice received 70% of the amount of food consumed by their respective AL-fed mice the previous day. Body fat (%) and bone mineral density (BMD) and content (BMC) were determined by PIXImus densitometry. There were strain-dependent effects on body mass, crown-to-rump length, percent body fat, and total body, femoral, and vertebral BMD and BMC under all conditions. SENCAR mice were heavier, longer, had larger bones, and generally exhibited higher total body, femoral, and vertebral BMC and BMD than C57 and DBA mice. DR had beneficial effects on BMD and BMC in the vertebrae of the SENCAR mouse model of high free radical generation and in the obese, diabetes-prone C57 mouse model of high end-stage protein glycation. DR DBA and SENCAR mice had lower femoral BMDs and BMCs than their respective AL-fed controls. Regression analysis confirmed linear relationships between total and lean body mass and total body and femoral BMDs and BMCs, suggesting that physiologic adaptation to a lower body mass accounts for the lower femoral bone mineral values observed in DR versus AL-fed mice. Thus, both hypotheses are, at least, partially valid. DR is beneficial in the trabeculae-rich vertebrae of animal models of high oxidant stress, and total/lean body mass determines BMD and BMC in the weight-bearing femur in DR and AL-fed mice.

摘要

饮食限制(DR)通过限制自由基生成和氧化损伤,在一定程度上延长了寿命并延缓了衰老。DR还会降低体重,而体重是影响整个生命周期骨量的一个主要决定因素。我们检验了这样一个假设,即与“负重部位的骨量由DR和自由采食(AL)喂养小鼠的体重决定”这一假设相比,DR对自由基生成量高的小鼠品系(对致癌作用敏感程度为SENCAR > C57 > DBA)的骨骼具有最有益的影响。每个品系的雄性小鼠在10周龄时(t(0))处死,或随机分为自由采食组或30%饮食限制组,喂养6个月。每天测量自由采食组小鼠的食物消耗量,饮食限制组小鼠则给予前一天各自自由采食组小鼠食物消耗量的70%。通过PIXImus骨密度仪测定体脂百分比、骨矿物质密度(BMD)和骨矿物质含量(BMC)。在所有条件下,体重、冠臀长度、体脂百分比以及全身、股骨和椎骨的BMD和BMC均存在品系依赖性效应。与C57和DBA小鼠相比,SENCAR小鼠更重、更长,骨骼更大,全身、股骨和椎骨的BMC和BMD通常更高。饮食限制对自由基生成量高的SENCAR小鼠模型的椎骨以及晚期蛋白糖基化程度高的肥胖、易患糖尿病的C57小鼠模型的BMD和BMC具有有益影响。饮食限制的DBA和SENCAR小鼠的股骨BMD和BMC低于各自自由采食组的对照小鼠。回归分析证实了总体重和瘦体重与全身及股骨BMD和BMC之间的线性关系,这表明对较低体重的生理适应解释了饮食限制组小鼠股骨骨矿物质值低于自由采食组小鼠的原因。因此,这两个假设至少部分是正确的。饮食限制对高氧化应激动物模型富含小梁骨的椎骨有益,而总体重/瘦体重决定了饮食限制组和自由采食组小鼠负重股骨的BMD和BMC。

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