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亚慢性砷暴露诱导中年大鼠骨骼肌萎缩和促红细胞生成素敏感性降低与血清褪黑素水平下降有关。

Subchronic Arsenite Exposure Induced Atrophy and Erythropoietin Sensitivity Reduction in Skeletal Muscle Were Relevant to Declined Serum Melatonin Levels in Middle-Aged Rats.

作者信息

Chen Xiong, Chen Wanying, Wang Dapeng, Ma Lu, Tao Junyan, Zhang Aihua

机构信息

The Key Laboratory of Environmental Pollution Monitoring and Disease Control, Ministry of Education, School of Public Health, Guizhou Medical University, Guiyang 550025, China.

出版信息

Toxics. 2023 Aug 10;11(8):689. doi: 10.3390/toxics11080689.

Abstract

Arsenic is a kind of widespread environmental toxicant with multiorgan-toxic effects, and arsenic exposure is associated with the occurrence and development of many chronic diseases. The influence of environmental arsenic exposure on skeletal muscle, which is a vital organ of energy and glucose metabolism, has received increasing attention. This study aimed to investigate the types of inorganic arsenic-induced skeletal muscle injury, and the potential regulatory effects of melatonin (MT) and erythropoietin (EPO) in young (3-month-old) and middle-aged (12-month-old) rats. Our results showed that 1 mg/L sodium arsenite exposure for 3 months could accelerate gastrocnemius muscle atrophy and promote the switch of type II fibers to type I fibers in middle-aged rats; however, it did not cause significant pathological changes of gastrocnemius muscle in young rats. In addition, arsenite could inhibit serum MT levels, and promote serum EPO levels but inhibit EPO receptor (EPOR) expression in gastrocnemius muscle in middle-aged rats, while serum MT levels and EPOR expression in gastrocnemius muscle showed an opposite effect in young rats. Importantly, exogenous MT antagonized the arsenite-induced skeletal muscle toxic effect and restored serum EPO and gastrocnemius muscle EPOR expression levels in middle-aged rats. There was a positive correlation among gastrocnemius muscle index, serum MT level, and gastrocnemius muscle EPOR protein level in arsenite-exposed rats. This study demonstrated that inorganic arsenic could accelerate skeletal muscle mass loss and type II fiber reduction in middle-aged rats, which may be related to decreased MT secretion and declined EPO sensitivity in skeletal muscle.

摘要

砷是一种广泛存在的环境毒物,具有多器官毒性作用,砷暴露与许多慢性疾病的发生发展相关。环境砷暴露对骨骼肌(能量和葡萄糖代谢的重要器官)的影响日益受到关注。本研究旨在探讨无机砷诱导的骨骼肌损伤类型,以及褪黑素(MT)和促红细胞生成素(EPO)对年轻(3月龄)和中年(12月龄)大鼠的潜在调节作用。我们的结果表明,1 mg/L亚砷酸钠暴露3个月可加速中年大鼠腓肠肌萎缩,并促进II型纤维向I型纤维转换;然而,它并未引起年轻大鼠腓肠肌的明显病理变化。此外,亚砷酸盐可抑制中年大鼠血清MT水平,促进血清EPO水平,但抑制腓肠肌中EPO受体(EPOR)表达,而年轻大鼠血清MT水平和腓肠肌中EPOR表达则呈现相反的作用。重要的是,外源性MT拮抗了亚砷酸盐诱导的中年大鼠骨骼肌毒性作用,并恢复了血清EPO和腓肠肌EPOR表达水平。在亚砷酸盐暴露大鼠中,腓肠肌指数、血清MT水平和腓肠肌EPOR蛋白水平之间存在正相关。本研究表明,无机砷可加速中年大鼠骨骼肌质量丢失和II型纤维减少,这可能与骨骼肌中MT分泌减少和EPO敏感性下降有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/77c4/10458431/acc7c8ef69d7/toxics-11-00689-g001.jpg

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