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瘦素和骆驼奶可减轻自闭症大鼠模型中丙戊酸诱导的氧化应激状态和遗传毒性。

Leptin and camel milk abate oxidative stress status, genotoxicity induced in valproic acid rat model of autism.

机构信息

1 Pharmacology & Toxicology Department, Faculty of Pharmacy, Fayoum University, Fayoum, Egypt.

2 Oral Biology Department, Faculty Oral and Dental Medicine, Cairo University, Egypt.

出版信息

Int J Immunopathol Pharmacol. 2018 Jan-Dec;32:2058738418785514. doi: 10.1177/2058738418785514.

Abstract

The aspect of treatment of autistic behaviour was investigated using valproic acid rat model of pregnant female rats. Two main groups (10 male rats/group) were treated for 6 days and then divided into six subgroups. The first group of normal rats was divided into three subgroups: (A) - control group, (B) - treated with camel milk (CAM; 2 mL/p.o) and (C) - treated with leptin (1000 µg/kg i.p) twice daily. The second group of autistic rats was randomly distributed into four subgroups as follows: (D) - positive control (autistics rats), (E) - treated with CAM, (F) - treated with a moderate dose of leptin and (G) - treated with a higher dose of leptin. Autistic behaviours of male offspring were checked by grooming and elevated pulz maze tests. Valproic acid (VPA)-induced autistic rats showed severe changes in oxidative stress markers, neurotransmitters and inflammatory cytokines, besides genotoxic manifestation of expression of tumour necrosis factor (TNF)-α, Bax and caspase-3. Leptin or CAM alone showed no signs of toxicity. CAM showed pronounced improvement in control rats than control itself. Leptin or CAM treatment of autistic animals showed a significant improvement of all measured parameters and genetic expression values. The improvement was pronounced in animals treated with CAM. These results suggest that CAM is a potential therapeutic candidate for autism via regulation of inflammatory and apoptotic pathways. Leptin plays an essential role in alleviation of autistic behaviour through antioxidant effects.

摘要

采用丙戊酸致孕大鼠模型研究了自闭症行为的治疗方法。将两组主要的雄性大鼠(每组 10 只)分别治疗 6 天,然后分为 6 个亚组。第一组正常大鼠分为三组:(A)-对照组,(B)-给予骆驼奶(CAM;2 mL/口服),(C)-给予瘦素(1000 µg/kg 腹腔注射),每日两次。第二组自闭症大鼠随机分为四组:(D)-阳性对照组(自闭症大鼠),(E)-给予 CAM,(F)-给予中等剂量瘦素,(G)-给予较高剂量瘦素。通过梳理和高架脉冲迷宫试验检查雄性后代的自闭症行为。丙戊酸(VPA)诱导的自闭症大鼠的氧化应激标志物、神经递质和炎性细胞因子发生严重变化,此外肿瘤坏死因子(TNF)-α、Bax 和 caspase-3 的表达也表现出遗传毒性。瘦素或 CAM 单独使用没有毒性迹象。CAM 对对照组大鼠的改善比对照组本身更明显。瘦素或 CAM 对自闭症动物的治疗显著改善了所有测量的参数和遗传表达值。用 CAM 治疗的动物的改善更为显著。这些结果表明,CAM 通过调节炎症和凋亡途径,是自闭症的一种潜在治疗候选药物。瘦素通过抗氧化作用在减轻自闭症行为方面发挥着重要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7914/6047246/7b3a08bc7fff/10.1177_2058738418785514-fig1.jpg

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