Katzman M A, Duffin J, Shlik J, Bradwejn J
Centre for Addiction and Mental Health-Clarke Division, Univerisyt of Toronto, Ontario, Canada.
Neuropsychopharmacology. 2002 Jun;26(6):824-31. doi: 10.1016/S0893-133X(02)00283-X.
The cholecystokinin (CCK) system, which has been shown to interact with both the panicogenic and respiratory systems, provides an interesting mechanism to further evaluate the central chemoreceptor and its effect on panic attack sensitivity. Intravenous CCK, a naturally occurring neuropeptide in the brain, has been found to induce the emotional and somatic symptoms of panic in both Panic Disorder (PD) and Normal Control (NC) subjects in a dose-dependent and reproducible fashion. To induce these effects, lower doses of intravenous CCK are required in the PD patients, relative to the NC subjects potentially suggesting that endogenous alterations in the CCK system may be contributing to the development of PD. Intravenous administration of CCK-4 in association with panic also results in subjective dyspnea, that is, diminution in vital capacity without an effect on the respiratory resistance. CCK-4 also causes a significant increase in tidal volume and minute ventilation but has no effect on breathing frequency. These observations suggest that a CCK-B receptor agonist may be acting as a respiratory stimulant, exerting its effect on anxiety through a direct effect on respiration. This study represents an examination of the specific effects of CCK-4 on the central chemoreceptor response. The study used a modified rebreathing technique, which accurately measures the ventilatory response to carbon dioxide in terms of both threshold and sensitivity. This technique requires the subject to rebreathe from a bag containing a hyperoxic and hypercapnic gas mixture resulting in rapid equilibration between alveolar gas and arterial blood. Use of a hyperoxic gas allows for the preferential examination of the central chemoreflexes (sensitive to CO(2)) with little if any effect of the peripheral (oxygen sensitive) chemoreflexes. After significant training, 15 healthy control subjects were assigned via a double blind procedure to receive an intravenous injection of placebo or CCK-4, using a between-subjects design. A between-subjects comparison was undertaken for the injection run (run #3) between subjects receiving the CCK-4 injection and those receiving the placebo injection. As well, a within-subject comparison was undertaken to compare the results of the run following the injection (run #3) vs. the previous run when no injection took place (run #2). No significant differences were noted between subjects who received CCK-4 as compared with placebo for: basal or sub-threshold ventilation, threshold CO(2) resulting in a change in ventilation, or sensitivity of the central chemoreflex, regardless of whether a panic attack did or did not take place. In addition, within the group receiving the CCK-4 challenge, no significant differences were noted during run #3 (received the CCK-4 injection) and a prior run where no injection took place (run #2). We conclude that CCK-4 does not act to induce panic by altering the central (CO(2) sensitive) chemoreceptor.
胆囊收缩素(CCK)系统已被证明与惊恐发作和呼吸系统相互作用,它为进一步评估中枢化学感受器及其对惊恐发作敏感性的影响提供了一个有趣的机制。静脉注射CCK是大脑中一种天然存在的神经肽,已发现它能以剂量依赖性和可重复的方式在惊恐障碍(PD)患者和正常对照(NC)受试者中诱发惊恐的情绪和躯体症状。为了诱发这些效应,相对于NC受试者,PD患者所需的静脉注射CCK剂量更低,这可能表明CCK系统的内源性改变可能促成了PD的发生。静脉注射CCK-4与惊恐发作相关时还会导致主观呼吸困难,即肺活量减小但对呼吸阻力无影响。CCK-4还会使潮气量和分钟通气量显著增加,但对呼吸频率无影响。这些观察结果表明,CCK-B受体激动剂可能作为一种呼吸兴奋剂,通过对呼吸的直接作用来影响焦虑。本研究旨在考察CCK-4对中枢化学感受器反应的具体影响。该研究采用了一种改良的重复呼吸技术,该技术能从阈值和敏感性两方面准确测量对二氧化碳的通气反应。该技术要求受试者从一个装有高氧和高碳酸气体混合物的袋子中重复呼吸,从而使肺泡气体和动脉血迅速达到平衡。使用高氧气体可优先检测中枢化学反射(对二氧化碳敏感),而对外周(对氧气敏感)化学反射的影响极小。经过大量训练后,15名健康对照受试者通过双盲程序被分配接受静脉注射安慰剂或CCK-4,采用组间设计。对接受CCK-4注射的受试者和接受安慰剂注射的受试者在注射阶段(第3阶段)进行组间比较。此外,还进行了受试者自身比较,以比较注射后阶段(第3阶段)与未注射的前一阶段(第2阶段)的结果。接受CCK-4的受试者与接受安慰剂的受试者在以下方面未发现显著差异:基础或阈下通气、导致通气变化的阈二氧化碳水平或中枢化学反射的敏感性,无论是否发生惊恐发作。此外,在接受CCK-4激发的组内,第3阶段(接受CCK-4注射)和未注射的前一阶段(第2阶段)之间未发现显著差异。我们得出结论,CCK-4不会通过改变中枢(对二氧化碳敏感)化学感受器来诱发惊恐发作。
