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Contrasting Effects of Increased and Decreased Dopamine Transmission on Latent Inhibition in Ovariectomized Rats and Their Modulation by 17β-Estradiol: An Animal Model of Menopausal Psychosis?

机译:多巴胺传递增加和减少对去卵巢大鼠潜伏抑制及其17β-雌二醇调节的对比作用:更年期精神病的动物模型?

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摘要

Women with schizophrenia have later onset and better response to antipsychotic drugs (APDs) than men during reproductive years, but the menopausal period is associated with increased symptom severity and reduced treatment response. Estrogen replacement therapy has been suggested as beneficial but clinical data are inconsistent. Latent inhibition (LI), the capacity to ignore irrelevant stimuli, is a measure of selective attention that is disrupted in acute schizophrenia patients and in rats and humans treated with the psychosis-inducing drug amphetamine and can be reversed by typical and atypical APDs. Here we used amphetamine (1 mg/kg)-induced disrupted LI in ovariectomized rats to model low levels of estrogen along with hyperfunction of the dopaminergic system that may be occurring in menopausal psychosis, and tested the efficacy of APDs and estrogen in reversing disrupted LI. 17β-Estradiol (50, 150 μg/kg), clozapine (atypical APD; 5, 10 mg/kg), and haloperidol (typical APD; 0.1, 0.3 mg/kg) effectively reversed amphetamine-induced LI disruption in sham rats, but were much less effective in ovariectomized rats; 17β-estradiol and clozapine were effective only at high doses (150 μg/kg and 10 mg/kg, respectively), whereas haloperidol failed at both doses. Haloperidol and clozapine regained efficacy if coadministered with 17β-estradiol (50 μg/kg, an ineffective dose). Reduced sensitivity to dopamine (DA) blockade coupled with spared/potentiated sensitivity to DA stimulation after ovariectomy may provide a novel model recapitulating the combination of increased vulnerability to psychosis with reduced response to APD treatment in female patients during menopause. In addition, our data show that 17β-estradiol exerts antipsychotic activity.
机译:在生殖年期间,精神分裂症妇女的发病较男性晚,对抗精神病药物(APDs)的反应更好,但绝经期与症状严重程度增加和治疗反应降低有关。已经提出雌激素替代疗法是有益的,但是临床数据不一致。潜在抑制(LI)是忽略无关刺激的能力,是一种选择性注意的措施,在急性精神分裂症患者以及用精神病诱导药物苯丙胺治疗的大鼠和人类中被破坏,并且可以被典型的和非典型的APD逆转。在这里,我们使用苯丙胺(1 µmg / kg)在去卵巢大鼠中诱导的LI破坏来模拟低水平的雌激素以及更年期精神病中可能发生的多巴胺能系统功能亢进,并测试了APD和雌激素逆转LI的功效。 17β-雌二醇(50、150μg / kg),氯氮平(非典型APD; 5、10μmg / kg)和氟哌啶醇(典型APD; 0.1、0.3μmg / kg)有效地逆转了安非他明引起的假性大鼠的LI破坏。在去卵巢大鼠中疗效较差; 17β-雌二醇和氯氮平仅在高剂量(分别为150μg/ kg和10μmg/ kg)下有效,而氟哌啶醇在两种剂量下均无效。如果与17β-雌二醇(50μg/ kg,无效剂量)合用,氟哌啶醇和氯氮平可恢复疗效。卵巢切除术后对多巴胺(DA)阻滞的敏感性降低,再加上对DA刺激的备用/增强敏感性,可能提供一种新颖的模型,概括了绝经期女性患者精神病易感性增加与对APD治疗反应降低的组合。另外,我们的数据表明17β-雌二醇发挥抗精神病活性。

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