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大鼠脊髓横断诱导溴隐亭降压作用增强:脊髓多巴胺受体的作用

Increase in the hypotensive effect of bromocriptine induced by spinal transection in rats: contribution of spinal dopamine receptors.

作者信息

Lahlou S, Demenge P

机构信息

Laboratoire de Physiologie Pharmacologie II, URA CNRS 1287, Faculté de Pharmacie, Université Joseph Fourier, Grenoble, France.

出版信息

J Cardiovasc Pharmacol. 1992 May;19(5):723-31.

PMID:1381770
Abstract

Intravenous (i.v.) administration of bromocriptine (150 micrograms/kg) in conscious normotensive rats with chronic spinal cord transection (at T5-T7), pretreated or not with i.v. propranolol (0.5 mg/kg), induced significant decreases in mean arterial blood pressure (MAP) which were greater and longer lasting than those in intact rats (-15 to -20 as compared with -10 mm Hg) for 8 days after transection. To assess the spinal and/or peripheral origin of this phenomenon, rats were also pretreated with either i.v. (0.3 mg/kg) or intrathecal (i.t.; 93 nmol/rat; at T9-T10) administration of domperidone, a selective dopamine (DA)2 receptor antagonist incapable of crossing the blood-brain barrier (BBB) freely. The increase in hypotension induced by spinal section was suppressed by i.t. but not by i.v. domperidone. In intact rats, bromocriptine elicited an increase in heart rate (HR; approximately 50 beats/min more), which was prevented by i.v. propranolol treatment. In spinal cord-transected rats, however, it had a significant bradycardic effect (approximately 50 beats/min less), which was antagonized by i.t.-administered domperidone. These results suggest that enhancement of the hypotensive effects induced by systemic administration of bromocriptine after a complete thoracic spinal transection is fully mediated by spinal DA2 receptors. This finding may help explain the increased orthostatic hypotension induced by DA receptor agonists in Parkinsonian patients with spinal lesions.

摘要

在慢性脊髓横断(T5 - T7)的清醒正常血压大鼠中,静脉注射溴隐亭(150微克/千克),无论是否预先静脉注射普萘洛尔(0.5毫克/千克),均可导致平均动脉血压(MAP)显著下降,与完整大鼠相比,横断后8天内下降幅度更大且持续时间更长(分别为-15至-20毫米汞柱和-10毫米汞柱)。为了评估这种现象的脊髓和/或外周起源,还对大鼠进行了预处理,分别静脉注射(0.3毫克/千克)或鞘内注射(i.t.;93纳摩尔/只;T9 - T10)多潘立酮,一种不能自由穿过血脑屏障(BBB)的选择性多巴胺(DA)2受体拮抗剂。脊髓横断引起的低血压增加被鞘内注射多潘立酮抑制,但静脉注射则无此作用。在完整大鼠中,溴隐亭引起心率(HR)增加(约多50次/分钟),静脉注射普萘洛尔治疗可预防。然而,在脊髓横断大鼠中,它具有显著的心动过缓作用(约少50次/分钟),鞘内注射多潘立酮可拮抗此作用。这些结果表明,在完全胸段脊髓横断后,全身给予溴隐亭引起的降压作用增强完全由脊髓DA2受体介导。这一发现可能有助于解释帕金森病脊髓损伤患者中DA受体激动剂引起的体位性低血压增加。

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