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精神分裂症及难治性精神分裂症中的内源性阿片系统:血浆内吗啡肽2、κ和μ阿片受体增加与白细胞介素-6相关。

The Endogenous Opioid System in Schizophrenia and Treatment Resistant Schizophrenia: Increased Plasma Endomorphin 2, and κ and μ Opioid Receptors Are Associated with Interleukin-6.

作者信息

Moustafa Shatha Rouf, Al-Rawi Khalid F, Stoyanov Drozdstoi, Al-Dujaili Arafat Hussein, Supasitthumrong Thitiporn, Al-Hakeim Hussein Kadhem, Maes Michael

机构信息

Clinical Analysis Department, College of Pharmacy, Hawler Medical University, Havalan City, Erbil 44001, Iraq.

College of Science, University of Anbar, Ramadi 31001, Iraq.

出版信息

Diagnostics (Basel). 2020 Aug 26;10(9):633. doi: 10.3390/diagnostics10090633.

DOI:10.3390/diagnostics10090633
PMID:32858974
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7554941/
Abstract

BACKGROUND

activation of the immune-inflammatory response system (IRS) and the compensatory immune-regulatory system (CIRS) plays a key role in schizophrenia (SCZ) and treatment resistant SCZ. There are only a few data on immune and endogenous opioid system (EOS) interactions in SCZ and treatment resistant SCZ.

METHODS

we examined serum β-endorphin, endomorphin-2 (EM2), mu-opioid (MOR) and kappa-opioid (KOR) receptors, and interleukin (IL)-6 and IL-10 in 60 non responders to treatment (NRTT), 55 partial RTT (PRTT) and 43 normal controls.

RESULTS

serum EM2, KOR, MOR, IL-6 and IL-10 were significantly increased in SCZ as compared with controls. β-endorphin, EM2, MOR and IL-6 were significantly higher in NRTT than in PRTT. There were significant correlations between IL-6, on the one hand, and β-endorphin, EM2, KOR, and MOR, on the other, while IL-10 was significantly correlated with MOR only. A large part of the variance in negative symptoms, psychosis, hostility, excitation, mannerism, psychomotor retardation and formal thought disorders was explained by the combined effects of EM2 and MOR with or without IL-6 while increased KOR was significantly associated with all symptom dimensions. Increased MOR, KOR, EM2 and IL-6 were also associated with neurocognitive impairments including in episodic, semantic and working memory and executive functions.

CONCLUSION

the EOS contributes to SCZ symptomatology, neurocognitive impairments and a non-response to treatment. In SCZ, EOS peptides/receptors may exert CIRS functions, whereas increased KOR levels may contribute to the pathophysiology of SCZ and EM2 and KOR to a non-response to treatment.

摘要

背景

免疫炎症反应系统(IRS)和代偿性免疫调节系统(CIRS)的激活在精神分裂症(SCZ)及难治性精神分裂症中起关键作用。关于精神分裂症及难治性精神分裂症中免疫与内源性阿片系统(EOS)相互作用的数据较少。

方法

我们检测了60例治疗无反应者(NRTT)、55例部分反应者(PRTT)和43例正常对照者的血清β-内啡肽、内吗啡肽-2(EM2)、μ-阿片受体(MOR)、κ-阿片受体(KOR)、白细胞介素(IL)-6和IL-10。

结果

与对照组相比,精神分裂症患者血清EM2、KOR、MOR、IL-6和IL-10显著升高。NRTT组的β-内啡肽、EM2、MOR和IL-6显著高于PRTT组。一方面,IL-6与β-内啡肽、EM2、KOR和MOR之间存在显著相关性,而IL-10仅与MOR显著相关。EM2和MOR联合或不联合IL-6的综合作用解释了阴性症状、精神病性症状、敌意、兴奋、怪癖、精神运动迟缓及形式思维障碍的大部分变异,而KOR升高与所有症状维度均显著相关。MOR、KOR、EM2和IL-6升高还与神经认知障碍有关,包括情景记忆、语义记忆、工作记忆及执行功能。

结论

内源性阿片系统导致精神分裂症的症状、神经认知障碍及治疗无反应。在精神分裂症中,内源性阿片系统肽/受体可能发挥代偿性免疫调节系统功能,而KOR水平升高可能促成精神分裂症的病理生理学,EM2和KOR则导致治疗无反应。

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