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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >ELECTROPHYSIOLOGICAL CHARACTERIZATION OF SPINAL NEURONS IN DIFFERENT MODELS OF DIABETES TYPE 1-AND TYPE 2-INDUCED NEUROPATHY IN RATS
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ELECTROPHYSIOLOGICAL CHARACTERIZATION OF SPINAL NEURONS IN DIFFERENT MODELS OF DIABETES TYPE 1-AND TYPE 2-INDUCED NEUROPATHY IN RATS

机译:糖尿病1型和2型糖尿病引起的神经病变的不同模型中脊髓神经的电生理特性

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摘要

Diabetic polyneuropathy (DPN) is a devastating complication of diabetes. The underlying pathogenesis of DPN is still elusive and an effective treatment devoid of side effects presents a challenge. There is evidence that in type-1 and -2 diabetes, metabolic and morphological changes lead to peripheral nerve damage and altered central nociceptive transmission, which may contribute to neuropathic pain symptoms. We characterized the electrophysiological response properties of spinal wide dynamic range (WDR) neurons in three diabetic models. The streptozotocin (STZ) model was used as a drug-induced model of type-1 diabetes, and the BioBreeding/Worcester (BB/Wor) and Zucker diabetic fatty (ZDF) rat models were used for genetic DPN models. Data were compared to the respective control group (BB/Wor diabetic-resistant, Zucker lean (ZL) and saline-injected Wistar rat). Response properties of WDR neurons to mechanical stimulation and spontaneous activity were assessed. We found abnormal response properties of spinal WDR neurons in all diabetic rats but not controls. Profound differences between models were observed. In BB/Wor diabetic rats evoked responses were increased, while in ZDF rats spontaneous activity was increased and in STZ rats mainly after discharges were increased. The abnormal response properties of neurons might indicate differential pathological, diabetes-induced, changes in spinal neuronal transmission. This study shows for the first time that specific electrophysiological response properties are characteristic for certain models of DPN and that these might reflect the diverse and complex symptomatology of DPN in the clinic. (C) 2015 IBRO. Published by Elsevier Ltd. All rights reserved.
机译:糖尿病多发性神经病(DPN)是糖尿病的毁灭性并发症。 DPN的潜在发病机理仍然难以捉摸,并且缺乏副作用的有效治疗方法也面临挑战。有证据表明,在1型和-2型糖尿病中,代谢和形态变化导致周围神经损伤和中枢伤害感受传递改变,这可能导致神经性疼痛症状。我们表征了三种糖尿病模型中脊髓宽动态范围(WDR)神经元的电生理反应特性。链脲佐菌素(STZ)模型被用作药物诱发的1型糖尿病模型,而BioBreeding / Worcester(BB / Wor)和Zucker糖尿病脂肪(ZDF)大鼠模型被用作遗传DPN模型。将数据与相应的对照组(BB / Wor糖尿病耐药,Zucker lean(ZL)和注射生理盐水的Wistar大鼠)进行比较。评估了WDR神经元对机械刺激和自发活动的反应特性。我们在所有糖尿病大鼠中发现了脊髓WDR神经元的异常反应特性,但没有发现对照。观察到模型之间的深刻差异。在BB / Wor糖尿病大鼠中,诱发反应增加,而在ZDF大鼠中,自发活动增加,而在STZ大鼠中,主要是在放电后增加。神经元的异常响应特性可能表明脊髓神经元传递存在差异性病理变化,糖尿病引起的变化。这项研究首次显示特定电生理反应特性是某些DPN模型的特征,并且可能反映了DPN在临床上的多种多样和复杂的症状。 (C)2015年IBRO。由Elsevier Ltd.出版。保留所有权利。

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