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静脉注射和脑室内注射食欲素-1(食欲素A)对食欲素受体-2基因突变发作性睡病犬的影响以及静脉注射食欲素-1替代疗法对一只缺乏食欲素配体的发作性睡病犬的影响。

Effects of IV and ICV hypocretin-1 (orexin A) in hypocretin receptor-2 gene mutated narcoleptic dogs and IV hypocretin-1 replacement therapy in a hypocretin-ligand-deficient narcoleptic dog.

作者信息

Fujiki Nobuhiro, Yoshida Yasushi, Ripley Beth, Mignot Emmanuel, Nishino Seiji

机构信息

Center for Narcolepsy, Stanford University School of Medicine, Palo Alto, CA 94304-5485, USA.

出版信息

Sleep. 2003 Dec 15;26(8):953-9. doi: 10.1093/sleep/26.8.953.

Abstract

STUDY OBJECTIVES

Using two different canine models of narcolepsy, we evaluated the therapeutic effects of hypocretin-1 on cataplexy and sleep.

MEASUREMENTS AND RESULTS

Intracerebroventricular administration of hypocretin-1 (10 and 30 nmol per dog) but not intravenous administration (up to 6 microg/kg) induced significant wakefulness in control dogs. However, hypocretin-1 had no effect on cataplexy or wakefulness in hypocretin receptor-2 gene (Hcrtr2) mutated narcoleptic Dobermans. Only very high intravenously doses of hypocretin-1 (96-384 microg/kg) penetrated the brain, to produce a short-lasting anticataplectic effect in a hypocretin-ligand-deficient animal.

CONCLUSIONS

Hypocretin-1 administration, by central and systemic routes, does not improve narcoleptic symptoms in Hcrtr2 mutated Dobermans. Systemic hypocretin-1 hardly crosses the blood-brain barrier to produce therapeutic effects. The development of more centrally penetrable and longer lasting hypocretin analogs will be needed to further explore this therapeutic pathway in humans.

摘要

研究目的

我们使用两种不同的发作性睡病犬模型,评估了食欲素-1对猝倒和睡眠的治疗效果。

测量与结果

向对照犬脑室内注射食欲素-1(每只犬10和30纳摩尔)可显著诱导清醒,但静脉注射(高达6微克/千克)则无此效果。然而,食欲素-1对食欲素受体-2基因(Hcrtr2)突变的发作性睡病杜宾犬的猝倒或清醒没有影响。只有非常高的静脉注射剂量的食欲素-1(96 - 384微克/千克)能够穿透血脑屏障,在缺乏食欲素配体的动物中产生短暂的抗猝倒作用。

结论

通过中枢和全身途径给予食欲素-1并不能改善Hcrtr2突变的杜宾犬的发作性睡病症状。全身给予的食欲素-1很难穿过血脑屏障产生治疗效果。需要开发更易穿透中枢且作用更持久的食欲素类似物,以进一步探索在人类中的这种治疗途径。

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