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精神分裂症的疼痛感知:神经肽、认知障碍和阴性症状的影响。

Pain perception in schizophrenia: influence of neuropeptides, cognitive disorders, and negative symptoms.

机构信息

Department of Affective and Psychotic Disorders, Medical University of Łódź, Łódź, Poland.

Department of Neurology and Movement Disorders, Medical University of Łódź, Łódź, Poland.

出版信息

Neuropsychiatr Dis Treat. 2015 Aug 6;11:2023-31. doi: 10.2147/NDT.S87666. eCollection 2015.

Abstract

OBJECTIVES

The causes and nature of insensitivity to pain in schizophrenia remain unknown. The role of endorphins and the association of cognitive dysfunction and negative symptoms are postulated.

METHODS

In this study, 43 patients with schizophrenia, five first-degree relatives, and 34 healthy controls were examined. Participants' plasma concentrations of substance P, β-endorphin, and calcitonin gene-related peptide (CGRP) were assessed. In patients, the Trail-Making Test, the Color Reading Interference Test (Stroop test), and the Positive and Negative Syndrome Scale Negative Syndrome subscale (PANSS N) test were performed. We also evaluated pain threshold using nociceptive reflex (RTIII) testing.

RESULTS

The mean β-endorphin concentration was about 20% higher in patients than in healthy controls (P<0.05). CGRP concentrations were significantly higher in patients than in controls (5.34 ng/mL versus 4.16 ng/mL; P<0.01). Subjects treated with antipsychotic polytherapy had higher concentrations of CGRP than did patients treated with second-generation antipsychotic monotherapy (5.92 ng/mL versus 5.02 ng/mL; P<0.05). There were no correlations between any biochemical parameters and Trail-Making Test, Stroop test, and PANSS N scores. There were no differences in RTIII among study groups. Strong negative correlation (P<0.001) was found between PANSS N scores and subjective pain threshold on the right lower limb.

CONCLUSION

The insensitivity to pain in schizophrenia is a complex phenomenon that is probably not related to changes in nociceptive pathways. Increase in β-endorphin level may be related to this issue, but it is uncertain if such concentration ensures analgesic effect. It is unknown if patients with schizophrenia in fact experience less pain. Cognitive impairment and excess negative symptoms may strongly influence the patient's expression of pain.

摘要

目的

精神分裂症患者痛觉迟钝的原因和性质尚不清楚。内啡肽的作用以及认知功能障碍和阴性症状的相关性被认为与之相关。

方法

本研究纳入了 43 名精神分裂症患者、5 名一级亲属和 34 名健康对照者。检测了参与者的血浆中 P 物质、β-内啡肽和降钙素基因相关肽(CGRP)的浓度。在患者中进行了连线测试、颜色阅读干扰测试(Stroop 测试)和阳性与阴性症状量表阴性症状子量表(PANSS N)测试。我们还使用伤害感受反射(RTIII)测试评估了疼痛阈值。

结果

患者的平均β-内啡肽浓度比健康对照组高约 20%(P<0.05)。患者的 CGRP 浓度明显高于对照组(5.34ng/mL 比 4.16ng/mL;P<0.01)。接受抗精神病药联合治疗的患者 CGRP 浓度高于接受第二代抗精神病药单药治疗的患者(5.92ng/mL 比 5.02ng/mL;P<0.05)。任何生化参数与连线测试、Stroop 测试和 PANSS N 评分均无相关性。研究组之间的 RTIII 无差异。PANSS N 评分与右侧下肢主观疼痛阈值之间存在强烈的负相关(P<0.001)。

结论

精神分裂症患者的痛觉迟钝是一种复杂的现象,可能与伤害感受通路的变化无关。β-内啡肽水平的增加可能与此问题有关,但尚不确定这种浓度是否能确保镇痛效果。尚不清楚精神分裂症患者是否实际上感到疼痛较少。认知障碍和过多的阴性症状可能会强烈影响患者对疼痛的表达。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b0d0/4532169/4c66177b7b38/ndt-11-2023Fig1.jpg

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