Seo Tomonori, Sumiyoshi Tomiki, Tsunoda Masahiko, Tanaka Kodai, Uehara Takashi, Matsuoka Tadasu, Itoh Hiroko, Kurachi Masayoshi
Department of Neuropsychiatry, University of Toyama Graduate School of Medicine and Pharmaceutical Sciences, Toyama, Japan.
Psychopharmacology (Berl). 2008 Apr;197(3):457-64. doi: 10.1007/s00213-007-1057-8. Epub 2008 Feb 5.
Neurodegenerative changes have been suggested to provide a basis for the pathophysiology of schizophrenia. T-817MA (1-{3-[2-(1-benzothiophen-5-yl) ethoxy] propyl} azetidin-3-ol maleate) is a novel compound with neuroprotective and neurite-outgrowth effects, as elicited in rat primary cultured neurons.
We examined the effect of T-817MA on phencyclidine (PCP)-induced disruption of prepulse inhibition (PPI), a measure of sensorimotor gating, in male Wistar rats.
In chronic experiments, male Wistar rats were injected intermittently with PCP (2.0 mg/kg, i.p., three times per week) or vehicle (saline, 2.0 ml/kg) for 1 month. T-817MA (0.21 or 0.07 mg/ml, p.o.) or distilled water was administered throughout the study period. In an acute experiment, T-817MA (8.4 mg/kg, p.o.) or distilled water was administered, followed by treatment with PCP (2.0 mg/kg, i.p.) or vehicle (saline, 2.0 ml/kg), before PPI measurements.
Intermittent administration of PCP for 1 month induced persistent disruption of PPI. Coadministration of T-817MA at 0.21 mg/ml but not 0.07 mg/ml completely blocked PCP-induced disruption of PPI, whereas T-817MA (0.21 mg/ml) by itself did not show a significant effect on PPI in control rats. On the other hand, single administration of T-817MA did not affect PPI disruption by acute treatment with PCP.
These results suggest that T-817MA is effective in ameliorating sensorimotor gating deficits caused by chronic PCP treatment, possibly via neuroprotective actions. Our findings provide a novel therapeutic approach for patients with schizophrenia.
神经退行性变被认为为精神分裂症的病理生理学提供了基础。T - 817MA(1-{3-[2-(1-苯并噻吩-5-基)乙氧基]丙基}氮杂环丁烷-3-醇马来酸盐)是一种新型化合物,在大鼠原代培养神经元中具有神经保护和促进神经突生长的作用。
我们研究了T - 817MA对苯环己哌啶(PCP)诱导的雄性Wistar大鼠前脉冲抑制(PPI)破坏的影响,PPI是一种感觉运动门控的指标。
在慢性实验中,雄性Wistar大鼠每周三次腹腔注射PCP(2.0 mg/kg)或溶剂(生理盐水,2.0 ml/kg),持续1个月。在整个研究期间给予T - 817MA(0.21或0.07 mg/ml,口服)或蒸馏水。在急性实验中,给予T - 817MA(8.4 mg/kg,口服)或蒸馏水,然后在测量PPI之前用PCP(2.0 mg/kg,腹腔注射)或溶剂(生理盐水,2.0 ml/kg)进行处理。
间歇性给予PCP 1个月可导致PPI持续破坏。联合给予0.21 mg/ml而非0.07 mg/ml的T - 817MA可完全阻断PCP诱导的PPI破坏,而单独的T - 817MA(0.21 mg/ml)对对照大鼠的PPI没有显著影响。另一方面,单次给予T - 817MA不影响急性PCP处理引起的PPI破坏。
这些结果表明,T - 817MA可能通过神经保护作用有效改善慢性PCP治疗引起的感觉运动门控缺陷。我们的发现为精神分裂症患者提供了一种新的治疗方法。
