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硝苯地平对环孢素相关性高血压的全身及肾脏影响。

Systemic and renal effects of nifedipine in cyclosporine-associated hypertension.

作者信息

Textor S C, Schwartz L, Wilson D J, Wiesner R, Romero J C, Augustine J, Kos P, Hay E, Gores G, Dickson E R

机构信息

Department of Medicine, Mayo Clinic, Rochester, MN 55905.

出版信息

Hypertension. 1994 Jan;23(1 Suppl):I220-4. doi: 10.1161/01.hyp.23.1_suppl.i220.

DOI:10.1161/01.hyp.23.1_suppl.i220
PMID:8282363
Abstract

Cyclosporine induces hypertension and wide-spread vasoconstriction after transplantation in addition to reducing kidney function. We studied hemodynamic, renal, and hormonal effects of monotherapy with nifedipine XL (n = 37) in liver transplant recipients within a year after transplant (median, 4.4 months). Systemic hemodynamics were determined with thoracic electrical bioimpedance. Blood pressure before therapy was 172 +/- 4/108 +/- 2 mm Hg. Sixty-four percent of recipients achieved blood pressures less than 140/90 mm Hg mediated by a fall in systemic vascular resistance index (2427 +/- 245 dyne.s.cm-5.m-2 in responders versus 2905 +/- 281 in nonresponders, P < .01). Despite the fall in systemic vascular resistance, glomerular filtration rates were not changed during nifedipine therapy, as measured by both creatinine and iothalamate clearances. Urinary prostacyclin (6-ketoprostaglandin F1 alpha) was suppressed below normal from 2468 +/- 323 ng/d before transplant to 1103 +/- 99 ng/d (P < .01) after transplant and did not change during nifedipine therapy. Urinary thromboxane B2 and plasma renin activity also fell after transplant and remained low during nifedipine. These data demonstrate that nifedipine can reverse systemic vasoconstriction associated with hypertension after transplantation. Systemic effects were not transmitted to the kidney sufficiently to improve glomerular filtration rate or reverse hormonal changes within the kidney. Hence, vascular and functional regulation of the kidney was dissociated from the systemic circulation during nifedipine administration after transplantation.

摘要

除降低肾功能外,环孢素在移植后还会引发高血压和广泛的血管收缩。我们研究了硝苯地平控释片单药治疗(n = 37)对肝移植受者在移植后一年内(中位数为4.4个月)的血流动力学、肾脏和激素方面的影响。采用胸部电阻抗法测定全身血流动力学。治疗前血压为172±4/108±2 mmHg。64%的受者通过降低全身血管阻力指数使血压降至140/90 mmHg以下(反应者的全身血管阻力指数为2427±245达因·秒·厘米⁻⁵·米⁻²,无反应者为2905±281,P <.01)。尽管全身血管阻力下降,但在硝苯地平治疗期间,通过肌酐清除率和碘肽酸盐清除率测定,肾小球滤过率并未改变。尿前列环素(6-酮-前列腺素F1α)从移植前的2468±323 ng/d被抑制至低于正常水平,移植后为1103±99 ng/d(P <.01),且在硝苯地平治疗期间未发生变化。移植后尿血栓素B2和血浆肾素活性也下降,并在硝苯地平治疗期间维持在低水平。这些数据表明,硝苯地平可逆转移植后与高血压相关的全身血管收缩。全身效应未充分传递至肾脏以改善肾小球滤过率或逆转肾脏内的激素变化。因此,移植后给予硝苯地平期间,肾脏的血管和功能调节与体循环分离。

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Metabolic complications in liver transplant recipients.肝移植受者的代谢并发症
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