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人脑内多巴胺D2受体结合与对疼痛刺激的反应及疼痛调节能力相关。

Dopamine D2 receptor binding in the human brain is associated with the response to painful stimulation and pain modulatory capacity.

作者信息

Hagelberg Nora, Martikainen Ilkka K, Mansikka Heikki, Hinkka Susanna, Någren Kjell, Hietala Jarmo, Scheinin Harry, Pertovaara Antti

机构信息

Department of Anaesthesiology and Intensive Care, University of Turku, Turku, Finland.

出版信息

Pain. 2002 Sep;99(1-2):273-9. doi: 10.1016/s0304-3959(02)00121-5.

Abstract

The pain modulatory role of dopamine D2 receptors of the human forebrain was studied by determining the association between dopamine D2 receptor binding potential and the response to experimental pain. Nineteen healthy male volunteers participated in a dopamine D2 receptor positron emission tomography study. The extrastriatal regions of interest studied with [11C]FLB 457 as radioligand (n = 11) were the anterior cingulum, the medial and lateral thalamus, the medial and lateral frontal cortex, and the medial and lateral temporal cortex. The striatal regions of interest studied with [11C]raclopride (n = 8) were the caudate nucleus and the putamen. The latency to the ice water-induced cold pain threshold and tolerance were determined in a separate psychophysical test session. Moreover, the cutaneous heat pain threshold and its elevation by concurrent cold pain in the contralateral hand were determined in each subject. Cold pain threshold was inversely correlated with D2 binding potential in the right putamen and the cold pain tolerance was inversely correlated with D2 binding potential in the right medial temporal cortex. The magnitude of heat pain threshold elevation induced by concurrent cold pain was directly correlated with D2 binding potential in the left putamen. Other correlations of D2 binding potentials in varying brain regions with sensory responses were not significant. A psychophysical control study (n = 10) showed that cold pain responses were identical in the right and left hand. The results indicate that dopamine D2 receptor binding potential in the human forebrain, particularly in the striatum, may be an important parameter in determining the individual cold pain response and the potential for central pain modulation. Accordingly, an individual with only few available D2 receptors in the forebrain is likely to have a high tonic level of pain suppression, combined with a low capacity to recruit more (dopaminergic) central pain inhibition by noxious conditioning stimulation.

摘要

通过确定多巴胺D2受体结合潜能与实验性疼痛反应之间的关联,研究了人类前脑多巴胺D2受体的疼痛调节作用。19名健康男性志愿者参与了一项多巴胺D2受体正电子发射断层扫描研究。以[11C]FLB 457作为放射性配体研究的纹外感兴趣区域(n = 11)包括前扣带回、内侧和外侧丘脑、内侧和外侧额叶皮质以及内侧和外侧颞叶皮质。以[11C]雷氯必利研究的纹状体感兴趣区域(n = 8)包括尾状核和壳核。在单独的心理物理学测试环节中确定冰水诱导的冷痛阈值和耐受性的潜伏期。此外,在每个受试者中测定皮肤热痛阈值及其因对侧手部同时存在的冷痛而升高的情况。冷痛阈值与右侧壳核中的D2结合潜能呈负相关,冷痛耐受性与右侧内侧颞叶皮质中的D2结合潜能呈负相关。同时存在的冷痛诱导的热痛阈值升高幅度与左侧壳核中的D2结合潜能呈正相关。不同脑区中D2结合潜能与感觉反应的其他相关性不显著。一项心理物理学对照研究(n = 10)表明,右手和左手的冷痛反应相同。结果表明,人类前脑,特别是纹状体中的多巴胺D2受体结合潜能可能是决定个体冷痛反应和中枢性疼痛调节潜能的一个重要参数。因此,前脑中只有少量可用D2受体的个体可能具有较高的紧张性疼痛抑制水平,同时通过有害条件刺激募集更多(多巴胺能)中枢性疼痛抑制的能力较低。

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