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哺乳期磺胺间甲氧嘧啶暴露对仔鼠骨骼肌蛋白质代谢及mTOR信号通路的影响
张强,刘开永
0
(安徽医科大学公共卫生学院;安徽医科大学公共卫生学院营养与食品卫生学)
摘要:
为了研究哺乳期磺胺间甲氧嘧啶(SMM)暴露对仔鼠骨骼肌蛋白质代谢及mTOR信号通路的影响,本实验以0、10、50、200 mg? kg-1?d-1剂量对哺乳期ICR小鼠灌胃给药直至出生后21天;第22天断乳时剖杀部分仔鼠,采集腓肠肌,BCA法测定其腓肠肌总蛋白含量,氨基酸分析仪测定其游离氨基酸水平,RT-PCR法检测其mTOR信号通路关键基因表达水平;另一部分仔鼠以性别分笼喂养至出生后63 d,并每周称重1次。与对照组比较,结果表明仔鼠体重无统计学差异(P > 0.05);中剂量组仔鼠腓肠肌谷氨酸(Glu), 甘氨酸(Gly), 丙氨酸(Ala), 瓜氨酸(Cit),蛋氨酸(Met)),组氨酸(His)和鹅肌肽(Ans)含量显著升高(P < 0.05);高剂量组的Cit和Ans含量也显著升高(P < 0.05),而低剂量组的Cit含量显著降低(P < 0.01);仔鼠腓肠肌Mtor, Pi3k3ca, Pi3k3cb, Akt1, Eif4ebp1和Rps6kb1等基因表达无统计学差异(P > 0.05);腓肠肌总蛋白含量无统计学差异(P > 0.05)。总之哺乳期SMM暴露对仔鼠骨骼肌氨基酸代谢有一定的改变作用;对 mTOR信号通路并未产生显著影响,为临床上探讨生命早期SMM暴露是否引起代谢性疾病问题提供了毒理学风险评估依据。
关键词:  哺乳期  磺胺间甲氧嘧啶(SMM)  骨骼肌  mTOR
DOI:
投稿时间:2015-11-22修订日期:2015-12-08
基金项目:国家自然科学基金项目(81202209);安徽省高等学校优秀青年人才基金(2012SQRL075ZD);安徽医科大学中青年学术骨干资助基金(2012051)
Effects of lactational exposure to sulfamonomethoxin on keletal muscle protein metabolism and mTOR signaling pathway in mice offspring
(School of Public Health,Anhui Medical University,An Hui Hefei 230601)
Abstract:
The aim of this study was to explore the effects of lactating mice exposed to sulfamonomethoxine (SMM) on skeletal muscle protein metabolism and the mTOR signaling pathway in offspring muscle. The lactating mice were gavaged with SMM (0, 10, 50, 200 mg? kg-1?d-1) for 21 days. On postnatal day (PND) 22, some of the offspring were sacrificed and the gastrocnemius muscles were collected. And then the other offspring were separated with gender, raised normally until PND 63, weighted once every week. The composition of free amino acids in muscle was analyzed by the automatic amino acid analyzer, the key gene expressions of mTOR pathway were quantitatively determined using real-time polymerase chain; Finally, the contents of total protein were determined by bicinchoninic acid method in muscle. Compared with controls, the exposure to SMM on body weight of the offspring made no significant difference during the experimental period (P>0.05). And at PND 22, the concentrations of Glu, Gly, Ala, Cit, Met, His and Ans were increased significantly in middle dose group (P<0.05), the ones of Cit and Ans were increased significantly at the high dose (P<0.05), but the one of Cit was notably decreased in the low dose group (P<0.01). The expressions of Mtor, Pi3k3ca, Pi3k3cb, Akt1, Eif4ebp1 and Rps6kb1 were not changed significantly (P>0.05). Moreover, the content of total protein in muscle were not changed in the treated groups. Together, lactating exposure to SMM altered the free amino acid profiling in offspring skeletal muscle, but the mTOR signaling pathway was not obviously affected, all of which will provide a scientific basis for toxiclogic risk assessment of causing metabolic problems when in early life exposure to SMM.
Key words:  Lactation  Sulfamonomethoxine (SMM)  Skeletal muscle  mTOR

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