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首页> 外文期刊>Bosnian Journal of Basic Medical Sciences >Lithium chloride could aggravate brain injury caused by 3-nitropropionic acid
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Lithium chloride could aggravate brain injury caused by 3-nitropropionic acid

机译:氯化锂可加重3-硝基丙酸引起的脑损伤

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Lithium, a well-known drug for the treatment of bipolar disorder, may also have the ability to reduce neurodegeneration and stimulate cell proliferation. Systemic injection of mitochondrial toxin 3-nitropropionic acid (3NPA) is known to induce a relatively selective, Huntington disease-like brain injury. The aim of this study was to determine the effect of lithium chloride (LiCl) on brain injury caused by 3NPA. Female adult Wistar rats were pre-treated with LiCl (127 mg/kg) 1 day before the first injection of 3NPA (28 mg/kg), and then for 8 days with the same treatment but receiving LiCl 1 hour before 3NPA. Control groups were pre-treated accordingly, with LiCl or with normal saline, but were not treated with 3NPA. Staining for cytochrome c oxidase activity and in situ hybridization autoradiography of synaptotagmin-4 and -7 mRNAs were used to evaluate brain injury caused by 3NPA. There was a significant reduction of body weight in the 3NPA+LiCl group (79%) compared to the 3NPA group (90%, p = 0.031) and both control groups (100%, p = 0.000). Densitometric evaluation of cytochrome c oxidase staining and in situ hybridization autoradiograms revealed that the pre-treatment with LiCl caused an increase in striatal lesion for about 40% ( p = 0.049). Moreover, the lesion was observed also in the hippocampus of three animals from the 3NPA+LiCl group and in two animals from the 3NPA group. However, there were no differences between the LiCl and saline group in any of the measured parameters. We concluded that the pre-treatment with a relatively nontoxic dose of LiCl could aggravate brain injury caused by 3NPA.
机译:锂,一种治疗双相情感障碍的著名药物,也可能具有减少神经变性和刺激细胞增殖的能力。全身注射线粒体毒素3-硝基丙酸(3NPA)会引起相对选择性的亨廷顿病样脑损伤。这项研究的目的是确定氯化锂(LiCl)对3NPA引起的脑损伤的作用。雌性成年Wistar大鼠在第一次注射3NPA(28 mg / kg)前1天用LiCl(127 mg / kg)进行预处理,然后进行8天相同处理,但在3NPA之前1小时接受LiCl。对照组相应地用LiCl或生理盐水进行了预处理,但未使用3NPA进行过治疗。染色的细胞色素c氧化酶活性和synaptotagmin-4和-7 mRNAs的原位杂交放射自显影用于评估3NPA引起的脑损伤。与3NPA组(90%,p = 0.031)和两个对照组(100%,p = 0.000)相比,3NPA + LiCl组的体重显着降低(79%)。细胞色素C氧化酶染色的密度测定评估和原位杂交放射自显影照片显示,用LiCl预处理可导致纹状体病变增加约40%(p = 0.049)。此外,在3NPA + LiCl组的三只动物和3NPA组的两只动物的海马中也观察到了病变。然而,在任何测量参数中,LiCl和盐水组之间没有差异。我们得出的结论是,使用相对无毒的LiCl进行预处理可能会加剧3NPA引起的脑损伤。

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