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心脏移植后环孢素A向他克莫司的转换。

Conversion of cyclosporine A to tacrolimus following heart transplantation.

作者信息

Mathieu P, Carrier M, White M, Pellerin M, Perrault L P, Pelletier G, Pelletier L C

机构信息

Montreal Heart Institute, Montreal, Canada.

出版信息

Can J Cardiol. 1999 Nov;15(11):1229-32.

Abstract

BACKGROUND

Cyclosporine A (CyA) is ususally the immunosuppressive drug of choice in organ transplantation; however, some side effects have limited its use. Tacrolimus is a novel immunosuppressive drug that is more potent than CyA, and has been used as a rescue agent following heart transplantation when the use of CyA is undesirable or inefficient.

PATIENTS AND METHODS

Since 1996, 14 heart transplant recipients under CyA were switched to tacrolimus therapy, for refractory rejection or intolerance, to conventional immunosuppression.

RESULTS

After a mean of 35+/-7 months of treatment, tacrolimus was substituted for CyA therapy. The reason for substitution was refractory rejection in six patients, gingival hypertrophy in five patients, hypertrichosis in one patient, severe arterial hypertension in one patient and hepatotoxicity in one patient. Five patients underwent a successful rescue therapy and one patient died of refractory rejection despite the use of tacrolimus. All patients with CyA side effects recovered with tacrolimus. After conversion from CyA to tacrolimus, the number of episodes of acute rejection decreased from a mean of 0.42+/-0.17 to 0.14+/-0.09 episodes/patient/month under CyA and tacrolimus therapy (P=0.11), respectively. The mean dose of prednisone was 0.18+/-0.06 mg/kg/day before compared with 0.06+/-0.01 mg/kg/day after conversion from CyA to tacrolimus (P=0.09). Creatinine serum levels averaged 124+/-7 mmol/L under CyA treatment compared with 113+/-7 mmol/L with tacrolimus therapy (P=0.002).

CONCLUSION

In patients with refractory rejections or intolerance to CyA after heart transplantation, conversion to tacrolimus-based immunosuppression is safe and effective.

摘要

背景

环孢素A(CyA)通常是器官移植中免疫抑制药物的首选;然而,一些副作用限制了其使用。他克莫司是一种新型免疫抑制药物,比CyA更有效,在心脏移植中当使用CyA不合适或无效时已被用作挽救药物。

患者和方法

自1996年以来,14例接受CyA治疗的心脏移植受者因难治性排斥反应或对传统免疫抑制不耐受而改用他克莫司治疗。

结果

经过平均35±7个月的治疗,他克莫司替代了CyA治疗。替代原因是6例患者难治性排斥反应,5例患者牙龈增生,1例患者多毛症,1例患者严重动脉高血压,1例患者肝毒性。5例患者接受了成功的挽救治疗,1例患者尽管使用了他克莫司仍死于难治性排斥反应。所有有CyA副作用的患者使用他克莫司后均康复。从CyA转换为他克莫司后,急性排斥反应发作次数分别从CyA治疗时的平均0.42±0.17次/患者/月降至他克莫司治疗时的0.14±0.09次/患者/月(P=0.11)。泼尼松的平均剂量在转换前为0.18±0.06mg/kg/天,从CyA转换为他克莫司后为0.06±0.01mg/kg/天(P=0.09)。CyA治疗时血清肌酐水平平均为124±7mmol/L,他克莫司治疗时为113±7mmol/L(P=0.002)。

结论

对于心脏移植后难治性排斥反应或对CyA不耐受的患者,转换为基于他克莫司的免疫抑制是安全有效的。

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