Piera M J, Beaughard M, Michelin M T, Massingham R
Riom Laboratoires-CERM, Service de Pharmacologie, France.
Arch Int Pharmacodyn Ther. 1995 May-Jun;329(3):347-59.
The effects of the 5-hydroxytryptamine1A agonists, 8-OH-DPAT, buspirone and flesinoxan, on the delayed hyperactivity and on the ensuing neuronal degeneration induced by transient global cerebral ischaemia, were studied. In normothermic, male Mongolian gerbils, subjected to 3 min bilateral carotid artery ligation, the locomotor activity was measured 1 day after ischaemia. The neuronal damage was quantified 7 days later using an image analysis system. Buspirone (3 and 10 mg/kg, i.p.) and flesinoxan (1 and 3 mg/kg, i.p.), administered twice a day for 3 days both in pre- and post-ischaemic conditions, failed to significantly protect the CA1 zone of the hippocampus against neuronal damage. In contrast, 8-OH-DPat (1 and 3 mg/kg, i.p.) significantly reduced the neuronal degeneration. All compounds abolished the hyperactivity but there was no correlation between this parameter and the extent of the reduction in neuronal damage. The ineffectiveness of buspirone and flesinoxan was not the result of too low a dose - as evidenced by the complete inhibition of hyperactivity with both compounds and by the appearance of a serotonin behavior syndrome with flesinoxan - but is possibly related to a partial agonist activity at the 5-hydroxytryptamine1A receptor, as reported for buspirone. Further studies are necessary to explain the differences between these agonists.
研究了5-羟色胺1A激动剂8-羟基二苯丙胺(8-OH-DPAT)、丁螺环酮和氟司必林对短暂性全脑缺血诱导的延迟性多动及随后的神经元变性的影响。在常温下,对雄性蒙古沙鼠进行3分钟双侧颈动脉结扎,缺血1天后测量其运动活性。7天后使用图像分析系统对神经元损伤进行量化。丁螺环酮(3和10毫克/千克,腹腔注射)和氟司必林(1和3毫克/千克,腹腔注射),在缺血前后均每天给药2次,持续3天,未能显著保护海马体CA1区免受神经元损伤。相比之下,8-OH-DPAT(1和3毫克/千克,腹腔注射)显著减少了神经元变性。所有化合物均消除了多动,但该参数与神经元损伤减少程度之间没有相关性。丁螺环酮和氟司必林无效并非剂量过低所致——这两种化合物对多动的完全抑制以及氟司必林出现5-羟色胺行为综合征证明了这一点——但可能与5-羟色胺1A受体的部分激动剂活性有关,如丁螺环酮所报道的那样。需要进一步研究来解释这些激动剂之间的差异。
