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A PET imaging study of 5-HT(1A) receptors in cat brain after acute and chronic fluoxetine treatment.

机译:急性和慢性氟西汀治疗后猫脑中5-HT(1A)受体的PET成像研究。

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摘要

Immuno-electron microscopic and beta-microprobe studies have demonstrated that the internalization of serotonin 5-HT(1A) autoreceptors, after acute treatment with the selective 5-HT(1A) receptor agonist 8-OH-DPAT or with the specific serotonin reuptake inhibitor (SSRI) fluoxetine, is associated with a marked decrease in the in vivo binding of [(18)F]MPPF in the nucleus raphe dorsalis (NRD) of rat. To determine whether this event might be amenable to brain imaging, the present [(18)F]MPPF positron emission tomographic (PET) study was carried out in anesthetized cats given or not a single dose (5 mg/kg, i.v.) or chronically treated with fluoxetine (5 mg/kg, s.c. for 21 days). Compared to control, [(18)F]MPPF binding potential was considerably (and visibly) decreased in the cat NRD after acute fluoxetine treatment, while it remained unchanged in other brain regions. Unexpectedly, after chronic fluoxetine treatment, [(18)F]MPPF binding potential was not affected in any brain region. In parallel immuno-electron microscopic experiments carried out in rat, the density of 5-HT(1A) autoreceptors on the plasma membrane of NRD dendrites was comparable to control after chronic fluoxetine treatment. If the decrease in [(18)F]MPPF binding at the onset of SSRI treatment was detectable by PET imaging, it could potentially serve as a biological index of efficacy.
机译:免疫电子显微镜和β-微探针研究表明,使用选择性5-HT(1A)受体激动剂8-OH-DPAT或特定5-羟色胺再摄取抑制剂进行急性治疗后,血清素5-HT(1A)自体受体的内在化(SSRI)氟西汀与大鼠核中缝背核(NRD)中[(18)F] MPPF的体内结合显着减少有关。为了确定该事件是否适合进行脑成像,本[[18] F] MPPF正电子发射断层扫描(PET)研究是在麻醉的猫中接受或不接受单剂量(5 mg / kg,iv)或长期服用的氟西汀(5 mg / kg,皮下注射21天)治疗。与对照组相比,在急性氟西汀治疗后的猫NRD中,[(18)F] MPPF的结合潜力显着(且明显)降低,而在其他脑区域则保持不变。出乎意料的是,在慢性氟西汀治疗后,[(18)F] MPPF结合潜力在任何大脑区域均不受影响。在大鼠中进行的并行免疫电子显微镜实验中,NRD树突质膜上5-HT(1A)自体受体的密度与慢性氟西汀治疗后的对照相当。如果通过PET成像可以检测到SSRI治疗开始时[(18)F] MPPF结合的减少,那么它有可能可以作为生物学功效指标。

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