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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Expression of NMDAR1, GluR1, GluR7, and KA1 glutamate receptor mRNAs is decreased in frontal cortex of 'neuroleptic-free' schizophrenics: evidence on reversible up-regulation by typical neuroleptics.
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Expression of NMDAR1, GluR1, GluR7, and KA1 glutamate receptor mRNAs is decreased in frontal cortex of 'neuroleptic-free' schizophrenics: evidence on reversible up-regulation by typical neuroleptics.

机译:NMDAR1,GluR1,GluR7和KA1谷氨酸受体mRNA的表达在“无神经痛症”精神分裂症的额叶皮层中减少:典型的精神抑制药可逆上调的证据。

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Schizophrenics exhibit abnormalities in many memory-associated functions mediated by the frontal cortex. Glutamate receptors play key roles in learning and memory. Hence, abnormalities in glutamate receptors within the frontal cortex may be associated with schizophrenia. In addition, emerging evidence indicates that glutamate receptors may be involved in the actions of antipsychotic drugs. To test these hypotheses, we measured mRNAs encoding the NMDAR1, GluR1, GluR7, and KA1 subunits of glutamate receptor in the left superior frontal gyrus from 21 elderly schizophrenics with varying histories of antipsychotic drug treatment and nine normal drug-free elderly controls. There were significant negative correlations between NMDAR1, GluR1, GluR7, and KA1 mRNA levels and time without neuroleptic medication before death in schizophrenics, indicating that levels of the glutamate receptor mRNAs decline rapidly after drug withdrawal. Further analysis revealed that in "neuroleptic-free" (>6 months) schizophrenics, levels of NMDAR1, GluR1, GluR7, and KA1 mRNAs were significantly lower than in controls. By contrast, in schizophrenics who were receiving neuroleptics until death, levels of NMDAR1, GluR1, GluR7, and KA1 mRNAs did not differ significantly from controls. These findings indicate that decreased levels of NMDAR1, GluR1, GluR7, and KA1 mRNAs may be present in the frontal cortex of some schizophrenics and that typical neuroleptics may reversibly increase levels of these mRNAs.
机译:精神分裂症在额叶皮层介导的许多记忆相关功能中表现出异常。谷氨酸受体在学习和记忆中起关键作用。因此,额叶皮层内谷氨酸受体的异常可能与精神分裂症有关。另外,新出现的证据表明谷氨酸受体可能与抗精神病药的作用有关。为了检验这些假设,我们测量了21名老年精神分裂症患者的左上额回中编码谷氨酸受体NMDAR1,GluR1,GluR7和KA1亚基的mRNA,这些抗精神病药物治疗的病史各不相同,还有9名正常的无药物老年对照。在精神分裂症患者死亡之前,NMDAR1,GluR1,GluR7和KA1 mRNA水平与不使用抗精神病药的时间之间存在显着的负相关性,这表明停药后谷氨酸受体mRNA的水平迅速下降。进一步的分析表明,在“无神经兴奋剂”(> 6个月)的精神分裂症中,NMDAR1,GluR1,GluR7和KA1 mRNA的水平显着低于对照组。相比之下,在接受抗精神病药物治疗直至死亡的精神分裂症患者中,NMDAR1,GluR1,GluR7和KA1 mRNA的水平与对照组无显着差异。这些发现表明,某些精神分裂症患者的额叶皮质中可能存在NMDAR1,GluR1,GluR7和KA1 mRNA降低的水平,典型的抗精神病药可能会可逆地增加这些mRNA的水平。

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