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清醒家兔对经皮硝酸甘油的反应存在压力反射重调定但无血管耐受性。

Baroreflex resetting but no vascular tolerance in response to transdermal glyceryl trinitrate in conscious rabbits.

作者信息

Serone A P, Angus J A, Wright C E

机构信息

Department of Pharmacology, University of Melbourne, Australia.

出版信息

Br J Pharmacol. 1996 May;118(1):93-104. doi: 10.1111/j.1476-5381.1996.tb15371.x.

Abstract
  1. We investigated whether acute (5 h) and chronic (3 days) transdermal glyceryl trinitrate (GTN) patches could cause the development of tolerance in terms of haemodynamics and vascular reactivity in the conscious rabbit. The effects of haemodynamic tolerance were assessed on arterial pressure, heart rate and the baroreflex control of heart rate, while hindquarter vascular reactivity in response to dilator and constrictor drugs and reactive hyperaemia were used to assess vascular tolerance. 2. Seven days prior to experiments, an inflatable cuff, a pulsed Doppler flow probe and an indwelling intra-aortic catheter (for i.a. agonist infusions) were implanted around the lower abdominal aorta. 3. In acute experiments, the effects of 0-5 h treatment with transdermal GTN (0 Sham), 10 or 20 mg 24 h-1) on MAP, HR and the baroreflex were examined. Chronic experiments were performed on three separated days (days 0 - before, 4 - with GTN patch and 8 - recovery). On each day, the baroreflex, reactive hyperaemic responses and hindquarter vascular dose-response curves to i.a. GTN, adenosine, acetylcholine, S-nitroso-N-acetylpenicillamine (SNAP) and methoxamine were assessed. On days 1-4, GTN was administered transdermally via a patch(es) (10 mg 24 h-1 (low dose) or 20 mg 24 h-1 (high dose); renewed every 24 h). 4. Acute treatment with 20 mg GTN 24 h-1, but not with 0 (n = 4) or 10 mg GTN 24 h-1 (n = 4), caused a significant fall in MAP (8 +/- 1 mmHg; n = 4) and resetting of the baroreflex by 5 h. Chronic GTN caused a significant fall in MAP of 8 +/- 2 and 8 +/- 2 mmHg on day 4 with low (n = 8) and high dose (n = 8), respectively, with no change in HR. There was no significant change to hindquarter vascular reactivity to i.a. infusion of GTN, nor were there any significant differences in the reactivity to i.a. adenosine, acetylcholine, SNAP or methoxamine with either low or high doses of GTN. 5. Chronic GTN treatment with low and high dose patches caused a parallel leftward shift ('resetting') of the baroreflex on day 4. By day 8, the baroreflex had still not recovered from this leftward shift 6. In the rabbit, chronic exposure to clinical nitrate patches caused haemodynamic compensation and baroreflex resetting but no evidence of vascular reactivity tolerance. Novel NO donor drugs and delivery regimens which provide intermittent dosing may prevent the development of haemodynamic resetting rather then preventing vascular tolerance, a commonly perceived difficulty in chronic nitrate therapy.
摘要
  1. 我们研究了急性(5小时)和慢性(3天)经皮硝酸甘油(GTN)贴片是否会在清醒兔的血流动力学和血管反应性方面导致耐受性的产生。通过动脉压、心率以及心率的压力反射控制来评估血流动力学耐受性的影响,而通过后肢血管对扩张剂和收缩剂药物的反应以及反应性充血来评估血管耐受性。2. 在实验前7天,在腹主动脉下部周围植入一个可充气袖带、一个脉冲多普勒血流探头和一根留置的主动脉内导管(用于主动脉内激动剂输注)。3. 在急性实验中,研究了经皮GTN(0(假手术)、10或20mg 24小时-1)0至5小时治疗对平均动脉压(MAP)、心率(HR)和压力反射的影响。慢性实验在三个不同的日子进行(第0天 - 之前、第4天 - 使用GTN贴片、第8天 - 恢复)。每天评估压力反射、反应性充血反应以及后肢血管对主动脉内GTN、腺苷、乙酰胆碱、S-亚硝基-N-乙酰青霉胺(SNAP)和甲氧明的剂量反应曲线。在第1至4天,通过贴片经皮给予GTN(10mg 24小时-1(低剂量)或20mg 24小时-1(高剂量);每24小时更换一次)。4. 24小时-1给予20mg GTN的急性治疗,但不是给予0(n = 4)或24小时-1给予10mg GTN(n = 4),导致MAP显著下降(8±1mmHg;n = 4),并在5小时时使压力反射重置。慢性GTN在第4天分别使低剂量组(n = 8)和高剂量组(n = 8)的MAP显著下降8±2和8±2mmHg,心率无变化。后肢血管对主动脉内输注GTN的反应性没有显著变化,低剂量或高剂量GTN对主动脉内腺苷、乙酰胆碱、SNAP或甲氧明的反应性也没有显著差异。5. 低剂量和高剂量贴片的慢性GTN治疗在第几天导致压力反射平行向左移位(“重置”)。到第8天,压力反射仍未从这种向左移位中恢复。6. 在兔中,长期暴露于临床硝酸酯贴片会导致血流动力学代偿和压力反射重置,但没有血管反应性耐受性的证据。提供间歇性给药的新型一氧化氮供体药物和给药方案可能会预防血流动力学重置的发生,而不是预防血管耐受性,这是慢性硝酸酯治疗中一个普遍认为的难题。

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