首页> 美国卫生研究院文献>Heliyon >Desipramine commonly used as a noradrenergic neuroprotectant in 6-OHDA-lesions leads to local functional changes in the urinary bladder and gastrointestinal tract in healthy rats
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Desipramine commonly used as a noradrenergic neuroprotectant in 6-OHDA-lesions leads to local functional changes in the urinary bladder and gastrointestinal tract in healthy rats

机译:Desipramine常用于6- OHDA-病变中的诺肾肾上腺素能神经保护剂导致尿膀胱和健康大鼠胃肠道的局部功能变化

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摘要

The 6-hydroxydopamine (6-OHDA) rat model is one of the most common animal models of Parkinson's disease. When experimentally inducing dopaminergic neurodegeneration in the nigrostriatal pathway using 6-OHDA, the noradrenergic reuptake inhibitor desipramine is often systemically injected in order to protect against damages to the noradrenergic system in the brain. An increasing number of studies are focusing on understanding the pathophysiological changes underlying autonomic non-motor symptoms, in particular urinary bladder and gastrointestinal dysfunctions, of the disease. Several of these studies have investigated the contractile properties and the activation of smooth muscle in the 6-OHDA rat model. Since the injection of desipramine is commonly placed in close proximity to the urinary bladder and gastrointestinal tract, in the current study we wanted to understand if the drug alone has an effect. For this, we have injected a single dose (25 mg/kg) of desipramine either intraperitonially or subcutaneously and investigated smooth muscle contractility in vitro in the urinary bladder, proximal colon and distal ileum four weeks post injection. Our data show that desipramine significantly alters smooth muscle contractility of the urinary bladder and proximal colon in healthy rats. Conclusively, we suggest, based on our data, that desipramine should be omitted when using the 6-OHDA rat model to investigate smooth muscle function in Parkinson's disease research.
机译:6-羟基戊胺(6-OHDA)大鼠模型是帕金森病的最常见的动物模型之一。在使用6-OHDA的Nigrostriatal途径中实验诱导多巴胺能神经变性的时,通常系统地注射脱脂症以防止对大脑中的诺肾上腺素能系统的损害。越来越多的研究专注于理解自主主义非运动症状,特别是疾病的膀胱和胃肠功能障碍的病理生理学变化。这些研究中的一些研究已经研究了6-OHDA大鼠模型中平滑肌的收缩性质和活化。由于甲醛注射通常靠近膀胱和胃肠道,因此在目前的研究中,我们希望理解单独的药物是否具有效果。为此,我们已经在注射后4周内在尿膀胱,近端结肠和远端感染性体外注射单剂量(25mg / kg)的甲醛和研究过的平滑肌收缩性。我们的数据显示,Desipramine显着改变了健康大鼠膀胱和近端结肠的平滑肌收缩性。结论,我们建议基于我们的数据,在使用6-OHDA大鼠模型中探讨帕金森病的平稳肌肉功能时,应省略甲状腺胺。

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