首页> 美国卫生研究院文献>other >Potassium Channel Antagonists 4-Aminopyridine and the T-Butyl Carbamate Derivative of 4-Aminopyridine Improve Hind Limb Function in Chronically Non-Ambulatory Dogs; A Blinded Placebo-Controlled Trial
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Potassium Channel Antagonists 4-Aminopyridine and the T-Butyl Carbamate Derivative of 4-Aminopyridine Improve Hind Limb Function in Chronically Non-Ambulatory Dogs; A Blinded Placebo-Controlled Trial

机译:钾通道拮抗剂4-氨基吡啶和4-氨基吡啶的氨基甲酸叔丁酯衍生物可改善非Non行犬的后肢功能;一项由安慰剂控制的盲法试验

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摘要

4-Aminopyridine (4-AP) blocks voltage gated potassium channels, restoring conduction to demyelinated axons and improving function in demyelinating conditions, but its use is associated with adverse effects and benefit in spinal cord injury is limited. Derivatives of 4-AP have been developed to improve clinical efficacy while reducing toxicity. We compared the therapeutic effects of orally administered 4-AP and its t-butyl carbamate derivative (t-butyl) with placebo in dogs that had suffered an acute spinal cord injury that left them chronically paralyzed. Nineteen dogs were entered into the trial, conducted in two-week treatment blocks starting with placebo, followed by random assignment to 4-AP or t-butyl, a washout and then the opposite medication followed by placebo. Investigators and owners were blinded to treatment group. Primary outcome measures included open field gait score (OFS), and treadmill based stepping score and regularity index, with additional secondary measures also considered. Thirteen of 19 dogs completed the protocol. Two were euthanized due to unrelated heath problems, two developed side effects and two were unable to complete for unrelated reasons. Dogs showed significant improvement in supported stepping score (from 17.39 to 37.24% with 4-AP; 16.85 to 29.18% with t-butyl p<0.0001) and OFS (from 3.63 to 4.73 with 4-AP; 3.78 to 4.45 with t-butyl, p = 0.005). Response was individually variable and most dramatic in three dogs that were able to walk without support with treatment. No significant difference was found between 4-AP and t-butyl. No adverse effects were reported with t-butyl but gastrointestinal upset and seizures were observed in two dogs with 4-AP. In conclusion, both 4-AP and t-butyl significantly improved supported stepping ability in dogs with chronic spinal cord injury with no adverse effects noted with t-butyl. Drug response varied widely between individuals, highlighting the need to understand the factors that influence canine and human patients' response to therapy.
机译:4-氨基吡啶(4-AP)阻断电压门控的钾离子通道,恢复脱髓鞘轴突的传导并改善脱髓鞘条件下的功能,但其使用会产生不良影响,并且对脊髓损伤的益处有限。已经开发了4-AP的衍生物以改善临床功效同时降低毒性。我们比较了口服4-AP及其氨基甲酸叔丁酯衍生物(叔丁基)与安慰剂对患有急性脊髓损伤并使其长期瘫痪的狗的治疗效果。 19只狗进入试验,从安慰剂开始为期两周的治疗,然后随机分配至4-AP或叔丁基,进行冲洗,然后再用相反的药物治疗,然后再使用安慰剂。研究者和所有者对治疗组视而不见。主要结局指标包括开放步态分数(OFS),基于跑步机的步伐分数和规律性指数,还考虑了其​​他辅助指标。 19只狗中有13只完成了实验方案。由于不相关的健康问题使两名安乐死,两名出现了副作用,而另两项由于不相关的原因而无法完成。狗的支撑步伐得分(4-AP从17.39降低到37.24%;叔丁基p <0.0001从16.85降低到29.18%)和OFS(4-AP从3.63降低到4.73;叔丁基从3.78降低到4.45有显着改善,p = 0.005)。响应是个体可变的,并且在三只能够在没有治疗的情况下行走的狗中最为显着。在4-AP和叔丁基之间没有发现显着差异。叔丁基没有不良反应的报道,但是胃肠道不适和两只患有4-AP的狗有癫痫发作。总之,在慢性脊髓损伤的狗中,4-AP和叔丁基均显着改善了支持的踩踏能力,而叔丁基未见不良反应。个体之间的药物反应差异很大,强调需要了解影响犬类和人类患者对治疗反应的因素。

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