[心脏移植后高脂血症能否得到最佳和安全的治疗?]。

Helvetica chirurgica acta Pub Date : 1994-12-01
K Wenke, J Thiery, N Arndtz, D Seidel, B Reichart
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引用次数: 0

摘要

“对于心脏移植后的高脂血症是否有安全且最佳的治疗方法?”心脏移植后高胆固醇血症的问题常常被低估。到目前为止,还没有治疗的概念,允许脂质参数的最佳调整。由于环孢素A相互作用、肝毒性和应用物质的效力有限,使用离子交换树脂、烟酸和贝特酸衍生物的治疗试验没有成功。在一项前瞻性、随机和对照试验中,我们研究了hmg -辅酶a还原酶抑制剂辛伐他汀对心脏移植受者的影响。研究纳入70例患者(辛伐他汀组37例,对照组33例)。8例患者在心脏移植后3个月内死亡。本研究的目的是将辛伐他汀治疗组的ldl -胆固醇值调整到<或= 110 mg/dl。治疗24个月后,平均ldl -胆固醇血浆水平为110 mg/dl。对照组相应的平均值为150 mg/dl。两组间差异有统计学意义(p < 0.001)。在同一时期,平均高密度脂蛋白胆固醇值增加了大约。两组均为15%(差异无统计学意义[p > 0.05])。辛伐他汀治疗组LDL/ hdl -胆固醇比值(2.28)显著低于对照组(2.94)(p < 0.05)。Lp(a)值差异无统计学意义。在24个月的观察期内,未观察到不良反应,特别是排斥反应发生率未增加。综上所述,我们推荐低剂量辛伐他汀治疗心脏移植后高胆固醇血症是一种安全和最佳的治疗方法。
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[Can hyperlipidemia after heart transplantation be optimally and safely treated?].

"Is there any safe and optimal treatment of hyperlipidemia following heart transplantation?" The problem of hypercholesterolemia following heart transplantation if often underestimated. Up to now there is no concept of therapy allowing an optimal adjustment of lipid parameters. Therapeutical trials using ion exchange resins, derivatives of nicotinic acids and fibrates were not successful due to cyclosporine A interaction, hepatotoxicity and limited efficacy of the applied substances. In a prospective, randomized and controlled trial we investigated the effects of the HMG-CoA-reductase inhibitor simvastatin in heart transplant recipients. The study included 70 patients (simvastatin n = 37, control group n = 33). 8 patients died within the first three months following heart transplantation. Purpose of the study was the adjustment of the LDL-cholesterol values in the simvastatin treated group to < or = 110 mg/dl. Following 24 months of treatment a mean LDL-cholesterol plasma level of 110 mg/dl was obtained. The corresponding mean value of the control group was 150 mg/dl. The difference between both groups was significant (p < 0.001). In the same period the mean HDL-cholesterol values increased by approx. 15% in both groups (no significant difference [p > 0.05]). The ratio of LDL/HDL-cholesterol was significant lower in the simvastatin treated group (2.28) than in the control group (2.94) (p < 0.05). There was no significant difference in Lp(a) values. No adverse side effects were observed within the observation period of 24 months, particularly no increase in the frequency of rejection episodes. Summarizing the above, we recommend low-dose simvastatin therapy as a safe and optimal treatment of hypercholesterolemia following heart transplantation.

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