Bone losses in obese, ovariectomized rats appear to be independent from sclerostin-induced inhibition of the Wnt/β-catenin pathway.

IF 1.2
Radosław Piotr Radzki, Marek Bieńko, Rafał Filip, Paweł Polak, Joanna Michalik Wolska
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引用次数: 4

Abstract

Introduction: Overweight and obesity, as well as a gonadal function, are pivotal factors influencing bone tissue metabolism.

Material and methods: The aim of the study was to determine the effect of dietary induced obesity (DIO) on bone tissue metabolism in sham-operated (SHO) or ovariectomized (OVX) adult female Wistar rats. Additionally, the influence of DIO in SHO or OVX on the concentration of sclerostin in the blood serum was analyzed. After SHO or OVX, the rats were placed in groups (n=8) and either received a standard diet (11.5 MJ/kg) (SHO-CON; OVX-CON) or a high-energy diet (17.6 MJ/kg) (SHO-FAT; OVX-FAT). The experiment lasted for 90 days and allowed for the establishment of osteopenia in OVX females and obesity in the rats that had received the high-energy diet.

Results: The results of the study demonstrate that obesity or/and ovariectomy increases the resorption of femora and tibiae, hence decreasing the densitometric and mechanical parameters affecting the bone structure in adult females rats. The strongest osteodegenerative effect was seen in the OVX-FAT females. Interestingly, the degree of bone tissue degradation caused exclusively by ovariectomy was similar to that found in the obese sham-operated rats.

Conclusions: Bone losses invoked by DIO seem to be independent from the Wnt/β-catenin pathway inhibition induced by sclerostin. While further study is necessary, the obtained results suggest that the usage of sclerostin anti-body in the treatment of osteoporosis can be ineffective, and in obese patients the undertaking of such therapy should be reassessed.

肥胖、去卵巢大鼠的骨质流失似乎与硬化蛋白诱导的Wnt/β-catenin通路的抑制无关。
超重和肥胖以及性腺功能是影响骨组织代谢的关键因素。材料与方法:研究膳食性肥胖(DIO)对假手术(SHO)或去卵巢(OVX)成年雌性Wistar大鼠骨组织代谢的影响。此外,还分析了SHO或OVX中DIO对血清中硬化素浓度的影响。在SHO或OVX后,将大鼠分组(n=8),每组给予标准日粮(11.5 MJ/kg) (SHO- con;OVX-CON)或高能量饮食(17.6 MJ/kg) (shoo - fat;OVX-FAT)。实验持续了90天,并允许在接受高能饮食的OVX雌性大鼠中建立骨质减少和肥胖。结果:研究结果表明,肥胖或/和卵巢切除增加了成年雌性大鼠股骨和胫骨的吸收,从而降低了影响骨结构的密度和力学参数。在OVX-FAT女性中观察到最强的骨退行性影响。有趣的是,完全由卵巢切除引起的骨组织退化程度与肥胖的假手术大鼠相似。结论:DIO引起的骨丢失似乎与硬化蛋白诱导的Wnt/β-catenin通路抑制无关。虽然需要进一步的研究,但所获得的结果表明,使用硬化蛋白抗体治疗骨质疏松症可能是无效的,在肥胖患者中应重新评估这种治疗的进行。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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