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首页> 外文期刊>Neurogastroenterology and motility >Colorectal distension-evoked potentials in awake rats: A novel method for studies of visceral sensitivity
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Colorectal distension-evoked potentials in awake rats: A novel method for studies of visceral sensitivity

机译:清醒大鼠大肠扩张诱发电位:一种研究内脏敏感性的新方法

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摘要

Background Quantification of the visceromotor response induced by colorectal distension (CRD) in rodents is commonly used for preclinical studies of visceral pain. The model is well established but does not fully assess the central response to stimulation. The aim of this study was to establish a novel model assessing cerebral evoked potentials (CEPs) in response to CRD in awake rats. Methods Epidural recording electrodes were chronically implanted in the skull of female Sprague-Dawley rats. Colorectal distension-induced CEPs were recorded using either rapid balloon distensions (100ms, 20-80mmHg) or electric stimulation (1ms, 1-4mA) using stimulation probes placed in the distal colon. Key Results Colorectal distension-induced CEPs were separated in three partly temporally overlapping components consisting of five prominent peaks. Peak latencies at 80mmHg were (P1, N1) 23±1 and 55±4ms, (N2, P2a, P2b) 91±3, 143±5 and 174±3ms, and (P3) 297±3ms. Amplitudes and latencies were, except for the early component, intensity dependent. Intrarectal administration of lidocaine significantly reduced the amplitude of N2 (by 42±6%, P<0.001) and P2 (by 34±6%, P<0.001). Electrically induced CEPs were intensity dependent and had similar topography and latencies as the mechanical evoked potentials (P1: 26±2ms; N1: 61±1ms; P2: 84±6ms; N2: 154±6ms; P3: 326±10ms), but there were large variations in amplitudes in between repeated electrical stimulations. Conclusions & Inferences Colorectal distension-induced CEPs can be recorded reliably in awake rats and may serve as a surrogate marker of colonic sensation and be a useful parameter in studies of visceral sensitivity.
机译:背景技术啮齿类动物中由结肠直肠扩张(CRD)引起的内脏运动反应的量化通常用于内脏痛的临床前研究。该模型已经建立,但是没有完全评估对刺激的中央反应。这项研究的目的是建立一种评估清醒大鼠响应CRD的脑诱发电位(CEP)的新型模型。方法将硬膜外记录电极长期植入雌性Sprague-Dawley大鼠的颅骨中。使用快速球囊扩张(100ms,20-80mmHg)或电刺激(1ms,1-4mA),使用放置在远端结肠中的刺激探针记录大肠扩张诱导的CEP。关键结果大肠扩张引起的CEPs分为三个在时间上重叠的部分,由五个突出峰组成。 80mmHg的峰值延迟为(P1,N1)23±1和55±4ms,(N2,P2a,P2b)91±3,143±5和174±3ms,(P3)297±3ms。除早期分量外,振幅和延迟与强度有关。利多卡因的直肠内给药显着降低了N2(降低42±6%,P <0.001)和P2(降低34±6%,P <0.001)的幅度。电诱发的CEP依赖于强度,并且具有与机械诱发电位相似的形貌和潜伏期(P1:26±2ms; N1:61±1ms; P2:84±6ms; N2:154±6ms; P3:326±10ms),但是重复电刺激之间的幅度有很大变化。结论与推论大肠扩张引起的CEPs可以在清醒的大鼠中可靠地记录,并且可以作为结肠感觉的替代标志物,并且是研究内脏敏感性的有用参数。

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