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Role of irisin in androgen-deficient muscle wasting and osteopenia in mice

机译:Irisin在雄激素缺乏肌肉丢失和小鼠骨质症的作用

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摘要

Androgen deficiency plays a crucial role in the pathogenesis of male osteoporosis and sarcopenia. Myokines have recently been identified as humoral factors that are involved in the interactions between muscle and bone; however, the influence of androgen deficiency on these interactions remains unclear. Therefore, we herein investigated the roles of humoral factors linking muscle to bone using orchidectomized mice with sarcopenia and osteopenia. Orchidectomy (ORX) significantly reduced muscle mass, grip strength, and trabecular bone mineral density (BMD) in mice. Among the myokines examined, ORX only significantly reduced fibronectin type III domain-containing 5 (Fndc5) mRNA levels in both the soleus and gastrocnemius muscles of mice. In simple regression analyses, Fndc5 mRNA levels in the soleus muscle positively correlated with trabecular BMD, but not cortical BMD. The administration of irisin, a product of Fndc5, significantly protected against the decrease induced in trabecular BMD, but not muscle mass, by androgen deficiency in mice. In conclusion, the present results demonstrated that androgen deficiency decreases the expression of irisin in the skeletal muscle of mice. Irisin may be involved in muscle/bone relationships negatively affected by androgen deficiency.
机译:雄激素缺乏在雄性骨质疏松症和康迟病的发病机制中起着至关重要的作用。最近被鉴定为肌肉和骨之间相互作用的体液因子;然而,雄激素缺乏对这些相互作用的影响仍不清楚。因此,我们在此研究了使用SARCOPENIA和骨核原瘤的植物联络小鼠将肌肉与骨骼连接到骨骼的体液因子的作用。植物切除术(ORX)显着降低了小鼠肌肉质量,握持强度和小梁骨密度(BMD)。在检查的肌肌内,ORX仅显着减少含有小鼠肌肉和腓肠肌肌肉中的含有III型型III结构域的5(FNDC5)mRNA水平。在简单的回归分析中,与小梁BMD的SOLEUS肌肉中的FNDC5 mRNA水平呈正相关,但不能皮质BMD。通过小梁BMD诱导的小梁BMD诱导的降低,伊森松施用IRISIN的给药显着保护,而不是小鸡缺乏肌肉质量。总之,目前的结果表明,雄激素缺乏减少了小鼠骨骼肌中鸢尾苷的表达。伊雷汀可能参与受雄激素缺乏影响的肌肉/骨骼关系。

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