Cremers T I, Wiersma L J, Bosker F J, den Boer J A, Westerink B H, Wikström H V
Department of Medicinal Chemistry, University of Groningen, Groningen, The Netherlands.
Biol Psychiatry. 2001 Jul 1;50(1):13-21. doi: 10.1016/s0006-3223(00)01093-3.
We investigated the combination of selective serotonin reuptake inhibitors (SSRIs) with the beta-adrenoceptor/serotonin 1A (5-HT(1A)) antagonist pindolol, based on the concept that 5-HT(1A) receptor blockade would eliminate the need for desensitization of presynaptic 5-HT(1A) receptors and therefore hasten the onset of action and improve the efficacy of SSRIs. However, since pindolol plasma levels after 2.5 mg three times a day are about 60 nmol/L, and the K(i) for the 5-HT(1A) receptor is 30 nmol/L, it is questionable whether pindolol levels in the brain would be sufficient to antagonize 5-HT(1A) receptors. Using microdialysis in the guinea pig, we correlated brain and plasma levels of pindolol with its capability of augmenting paroxetine-induced increases in brain 5-HT levels. In addition, central beta-receptor antagonism of pindolol was studied by investigating blockade of beta-agonist-induced increases in brain cyclic adenosine monophosphate (cAMP) formation.
Using microdialysis and jugular vein catheterization, we studied the ability of systemically administered pindolol to antagonize central 5-HT(1A) and beta-adrenoceptors, while simultaneously monitoring pindolol plasma and brain concentrations.
Augmentation of paroxetine-induced increases in extracellular 5-HT levels in the ventral hippocampus was only observed at steady state plasma levels exceeding 7000 nmol/L (concurrent brain levels 600 nmol/L). In contrast, antagonism of beta-agonist-induced increases of brain cAMP levels was already observed at pindolol plasma levels of 70 nmol/L (concurrent brain levels < 3 nmol/L).
At plasma levels that are observed in patients after 2.5 mg three times a day ( approximately 60 nmol/L), pindolol produces only a partial blockade of presynaptic 5-HT(1A) autoreceptors and does not augment the SSRI-induced 5-HT increase in the guinea pig brain. It is therefore very unlikely that the favorable effects of combining pindolol with SSRIs, as reported in a number of clinical studies, are due to 5-HT(1A) antagonism. Since pindolol completely blocks central beta-adrenoreceptors at clinically relevant plasma levels, it is possible that beta-adrenoceptor antagonism is involved in mediating pindolol's beneficial effects.
我们基于5-羟色胺1A(5-HT(1A))受体阻断可消除对突触前5-HT(1A)受体脱敏的需求,从而加速起效并提高选择性5-羟色胺再摄取抑制剂(SSRI)疗效的概念,研究了SSRI与β-肾上腺素能受体/5-羟色胺1A(5-HT(1A))拮抗剂吲哚洛尔的联合应用。然而,由于每日3次服用2.5mg吲哚洛尔后的血浆水平约为60nmol/L,而5-HT(1A)受体的解离常数(K(i))为30nmol/L,因此吲哚洛尔在脑内的水平是否足以拮抗5-HT(1A)受体存在疑问。我们在豚鼠中运用微透析技术,将吲哚洛尔的脑内和血浆水平与其增强帕罗西汀诱导的脑内5-羟色胺水平升高的能力进行关联。此外,通过研究对β-激动剂诱导的脑内环磷酸腺苷(cAMP)生成增加的阻断作用,对吲哚洛尔的中枢β受体拮抗作用进行了研究。
我们运用微透析和颈静脉插管技术,研究全身给予吲哚洛尔拮抗中枢5-HT(1A)和β-肾上腺素能受体的能力,同时监测吲哚洛尔的血浆和脑内浓度。
仅在稳态血浆水平超过7000nmol/L(同期脑内水平600nmol/L)时,才观察到吲哚洛尔增强了帕罗西汀诱导的腹侧海马细胞外5-羟色胺水平升高。相反,在吲哚洛尔血浆水平为70nmol/L(同期脑内水平<3nmol/L)时,就已观察到对β-激动剂诱导的脑内cAMP水平升高的拮抗作用。
在患者每日3次服用2.5mg(约60nmol/L)后所观察到的血浆水平下,吲哚洛尔仅对突触前5-HT(1A)自身受体产生部分阻断作用,且不会增强SSRI诱导的豚鼠脑内5-羟色胺升高。因此,一些临床研究中所报道的吲哚洛尔与SSRI联合应用的有益效果极不可能是由于5-HT(1A)拮抗作用。由于吲哚洛尔在临床相关血浆水平时可完全阻断中枢β-肾上腺素能受体,因此β-肾上腺素能受体拮抗作用可能参与介导了吲哚洛尔的有益效应。
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