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慢性使用第一代和第二代抗精神病药物后, Homer1a 基因的急性诱导模式得以保留:短期停药的影响及与 Homer1a 相互作用基因的比较。

Pattern of acute induction of Homer1a gene is preserved after chronic treatment with first- and second-generation antipsychotics: effect of short-term drug discontinuation and comparison with Homer1a-interacting genes.

机构信息

Laboratory of Molecular Psychiatry and Psychopharmacotherapy, Section of Psychiatry, Department of Neuroscience, University School of Medicine 'Federico II', Naples, Italy.

出版信息

J Psychopharmacol. 2011 Jul;25(7):875-87. doi: 10.1177/0269881109358199. Epub 2010 Feb 10.

DOI:10.1177/0269881109358199
PMID:20147574
Abstract

Homer1a is a glutamate-related gene whose expression is induced by antipsychotics acutely (i.e. 90 min after treatment). Acute Homer1a expression is preserved after prolonged antipsychotic treatments, while the effects of short-term discontinuation after chronic antipsychotic treatment have not yet been assessed. Here, we studied early and long-term effects on gene expression by antipsychotics for Homer1a and other components of glutamatergic synapses. In the first paradigm, we evaluated Homer1a acute expression by single administration of antipsychotics (haloperidol 0.8 mg/kg, ziprasidone 10 and 4 mg/kg, clozapine 15 mg/kg). Haloperidol and ziprasidone induced Homer1a in the striatum. Induction by ziprasidone was dose-dependent. These results suggest that acute Homer1a expression correlates with dopaminergic affinity and motor side effects of antipsychotics. In the second paradigm, we studied antipsychotic-mediated long-term changes in Homer1a and glutamate-related genes. Rats were treated (21 days) with haloperidol 0.8 mg/kg, ziprasidone 4 mg/kg, or vehicle, and then sacrificed at 90 min (early time-point) or 24 h (delayed time-point) after last injection. Gene expression at these two time-points was compared. Homer1a preserved its pattern of expression at the early but not at the delayed time-point. Significant changes were also observed for PSD-95. The results suggest that Homer1a preserves its expression profile after chronic antipsychotics.

摘要

Homer1a 是一种谷氨酸相关基因,其表达可被抗精神病药急性诱导(即在治疗后 90 分钟)。急性 Homer1a 表达在长期抗精神病治疗后得以保留,而慢性抗精神病治疗后短期停药的影响尚未评估。在这里,我们研究了抗精神病药对 Homer1a 和其他谷氨酸能突触成分的早期和长期基因表达的影响。在第一个范式中,我们通过单次给予抗精神病药(氟哌啶醇 0.8mg/kg、齐拉西酮 10 和 4mg/kg、氯氮平 15mg/kg)来评估 Homer1a 的急性表达。氟哌啶醇和齐拉西酮诱导纹状体中的 Homer1a。齐拉西酮的诱导作用呈剂量依赖性。这些结果表明,急性 Homer1a 表达与抗精神病药的多巴胺能亲和力和运动副作用相关。在第二个范式中,我们研究了抗精神病药介导的 Homer1a 和谷氨酸相关基因的长期变化。大鼠用氟哌啶醇 0.8mg/kg、齐拉西酮 4mg/kg 或载体处理 21 天,然后在最后一次注射后 90 分钟(早期时间点)或 24 小时(延迟时间点)处死。比较这两个时间点的基因表达。Homer1a 在早期保持其表达模式,但在延迟时间点则不然。PSD-95 也发生了显著变化。结果表明,慢性抗精神病药后 Homer1a 保留其表达谱。

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