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具有止吐特性的5-羟色胺3(5-HT3)受体拮抗剂GR 38032F对晕动病和动眼神经功能的影响。

The effect on motion sickness and oculomotor function of GR 38032F, a 5-HT3-receptor antagonist with anti-emetic properties.

作者信息

Stott J R, Barnes G R, Wright R J, Ruddock C J

机构信息

R.A.F. Institute of Aviation Medicine, Farnborough, Hampshire.

出版信息

Br J Clin Pharmacol. 1989 Feb;27(2):147-57. doi: 10.1111/j.1365-2125.1989.tb05345.x.

Abstract
  1. The 5-hydroxytryptamine (5-HT3) receptor antagonist, GR 38032F, which possesses potent anti-emetic properties in vomiting induced by cancer chemotherapeutic drugs, has been tested to determine its value in the prophylaxis of motion sickness induced by cross-coupled stimulation. The double-blind trial compared GR 38032F with both a placebo (lactose) and with hyoscine. In addition, studies of ocular pursuit and saccadic eye movements were carried out following the administration of each drug. 2. The prophylactic effect of GR 38032F on motion-induced nausea was indistinguishable from that of placebo, whereas following hyoscine subjects showed a highly significant (P less than 0.001) increase in tolerance to cross-coupled stimulation. Tests of oculomotor function showed no effect on saccadic eye movement from either drug. However, both drugs produced a significant (P less than 0.05) though small reduction in eye velocity gain during pursuit eye movement. 3. These findings suggest that the 5-HT3 receptor is not involved in the neural pathways that bring about motion sickness, but that it may have a role in the control of ocular pursuit. The absence of an anti-motion sickness effect from a drug that is effective in the treatment of vomiting induced by cancer chemotherapy serves to emphasize that different neural mechanisms are involved in the generation of motion sickness.
摘要
  1. 5-羟色胺(5-HT3)受体拮抗剂GR 38032F在癌症化疗药物所致呕吐中具有强效止吐特性,已对其在预防交叉耦合刺激引起的晕动病方面的价值进行了测试。双盲试验将GR 38032F与安慰剂(乳糖)以及东莨菪碱进行了比较。此外,在给予每种药物后还进行了眼球跟踪和扫视眼动研究。2. GR 38032F对运动诱发恶心的预防作用与安慰剂无异,而给予东莨菪碱后,受试者对交叉耦合刺激的耐受性显著提高(P小于0.001)。动眼功能测试表明,两种药物对扫视眼动均无影响。然而,两种药物在跟踪眼动期间均使眼球速度增益有显著(P小于0.05)但幅度较小的降低。3. 这些发现表明,5-HT3受体不参与引发晕动病的神经通路,但可能在眼球跟踪控制中起作用。一种对癌症化疗所致呕吐有效的药物却没有抗晕动病作用,这进一步强调了晕动病的发生涉及不同的神经机制。

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