In Vivo Protection against NMDA-induced Neurodegeneration by MK-801 and Nimodipine: Combined Therapy and Temporal Course of Protection

Stuiver B.T. , Douma B.R.K. , Bakker R. , Nyakas C. , Luiten P.G.M.
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引用次数: 65

Abstract

Neuroprotection against excitotoxicity by a combined therapy with the N-methyl-D-aspartate (NMDA) receptor antagonist MK-801 and the L-type Ca2+channel blocker nimodipine was examined using an in vivo rat model of NMDA-induced neurodegeneration. Attention was focused on the neuroprotective potential of this combined drug treatmentbeforeandafterNMDA-exposure. NMDA was unilaterally injected in the magnocellular nucleus basalis (MBN). Neuronal damage was assessed 12 days after the NMDA-injection by measuring the reduction of cholinergic cortical fibres that originate from the MBN neurons. In controls that received no drug treatment, NMDA-exposure damaged MBN neurons such that 66% of the cholinergic terminals were lost in the ipsilateral parietal cortex. Pretreatment with a nimodipine diet (860 ppm) combined with application of MK-801 (5 mg/kg i.p.)beforeNMDA-exposure reduced fibre loss by 89% thereby providing a near complete neuroprotection. Combined therapy of MK-801 (5 mg/kg i.p.) and nimodipine (15 mg/kg i.p.) 8 minafterNMDA-infusion reduced neuronal injury by 82%, while the same combination given 2 hafterthe excitotoxic treatment still yielded a 66% protection against neurotoxic damage invoked by NMDA. In conclusion, the present data show that a dual blockade of NMDA-channels and voltage-dependent calcium channels (VDCC's) up to 2 h after NMDA-exposure is able to provide a significant protection against NMDA-neurotoxicity.

MK-801和尼莫地平对nmda诱导的神经变性的体内保护作用:联合治疗和时间保护
采用NMDA诱导的神经变性大鼠模型,研究了n -甲基- d -天冬氨酸(NMDA)受体拮抗剂MK-801和l型Ca2+通道阻滞剂尼莫地平联合治疗对兴奋性毒性的神经保护作用。注意力集中在nmda暴露前后这种联合药物治疗的神经保护潜力上。在大细胞基底核(MBN)单侧注射NMDA。注射nmda后12天,通过测量源自MBN神经元的胆碱能皮质纤维的减少来评估神经元损伤。在未接受药物治疗的对照组中,nmda暴露损伤了MBN神经元,导致同侧顶叶皮层66%的胆碱能末梢丢失。在暴露于mda之前,用尼莫地平饮食(860 ppm)和MK-801 (5 mg/kg i.p)进行预处理,减少了89%的纤维损失,从而提供了近乎完全的神经保护。MK-801 (5 mg/kg i.p)和尼莫地平(15 mg/kg i.p)在NMDA输注8分钟后联合治疗可减少82%的神经元损伤,而在兴奋性毒性治疗2分钟后给予相同的联合治疗仍可对NMDA引起的神经毒性损伤产生66%的保护。总之,目前的数据表明,nmda暴露后长达2小时的nmda通道和电压依赖性钙通道(VDCC)的双重阻断能够提供对nmda神经毒性的显著保护。
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