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NMDA受体拮抗剂金刚烷胺和美金刚的脑渗透及体内回收率:一项定量微透析研究

Brain penetration and in vivo recovery of NMDA receptor antagonists amantadine and memantine: a quantitative microdialysis study.

作者信息

Hesselink M B, De Boer B G, Breimer D D, Danysz W

机构信息

Department of Pharmacological Research, Merz + Co., Frankfurt/Main, Germany.

出版信息

Pharm Res. 1999 May;16(5):637-42. doi: 10.1023/a:1018856020583.

Abstract

PURPOSE

To determine free brain concentrations of the clinically used uncompetitive NMDA antagonists memantine and amantadine using microdialysis corrected for in vivo recovery in relations to serum, CSF and brain tissue levels and their in vitro potency at NMDA receptors.

METHODS

Microdialysis corrected for in vivo recovery was used to determine brain ECF concentrations after steady-state administration of either memantine or amantadine. Additionally CSF, serum, and brain tissue were analyzed.

RESULTS

Following 7 days of infusion of memantine or amantadine (20 and 100 mg/kg/day respectively) whole brain concentrations were 44-and 16-fold higher than free concentrations in serum respectively. The free brain ECF concentration of memantine (0.83 +/- 0.05 microM) was comparable to free serum and CSF concentrations. In case of amantadine, it was lower. A higher in vivo than in vitro recovery was found for memantine.

CONCLUSIONS

At clinically relevant doses memantine reaches a brain ECF concentration in range of its affinity for the NMDA receptor and close to its free serum concentration. This is not the case for amantadine and different mechanisms of action may be operational.

摘要

目的

使用经体内回收率校正的微透析技术,测定临床使用的非竞争性N-甲基-D-天冬氨酸(NMDA)拮抗剂美金刚和金刚烷胺的游离脑浓度,该浓度与血清、脑脊液和脑组织水平相关,并测定它们在NMDA受体上的体外效力。

方法

使用经体内回收率校正的微透析技术,在美金刚或金刚烷胺稳态给药后测定脑细胞外液(ECF)浓度。此外,还对脑脊液、血清和脑组织进行了分析。

结果

在分别输注美金刚或金刚烷胺7天(分别为20和100mg/kg/天)后,全脑浓度分别比血清中的游离浓度高44倍和16倍。美金刚的游离脑ECF浓度(0.83±0.05μM)与游离血清和脑脊液浓度相当。对于金刚烷胺,其浓度较低。发现美金刚的体内回收率高于体外回收率。

结论

在临床相关剂量下,美金刚达到的脑ECF浓度在其对NMDA受体的亲和力范围内,且接近其游离血清浓度。金刚烷胺则并非如此,可能存在不同的作用机制。

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