Kaufman D B, Leventhal J R, Stuart J, Abecassis M M, Fryer J P, Stuart F P
Department of Surgery, Northwestern University Medical School, Chicago, Illinois 60611, USA.
Transplantation. 1999 Feb 27;67(4):586-93. doi: 10.1097/00007890-199902270-00017.
The current study examines the use of mycophenolate mofetil (MMF) and tacrolimus as primary immunosuppression in simultaneous pancreas-kidney (SPK) transplantation. In addition, analyses of the rates of conversion from one immunosuppressive agent to another, and its subsequent consequences with respect to outcomes were determined. Quality of graft function, infections, and effect on preexisting essential hypertension are also described.
Immunosuppression consisted of quadruple therapy with antithymocyte globulin induction, tacrolimus, MMF, and prednisone. Patient and graft survival and rejection rates in 50 consecutive SPK recipients, followed for a minimum of 3 months and a mean of 14 months (range: 3-34 months), are described.
Thirty-nine of 50 (78%) patients tolerated the MMF/tacrolimus combination long-term (mean duration of follow-up: 14+/-7 months). Nine of 50 patients (18%) were converted to Neoral, and 4 patients were converted to azathioprine as a substitute for MMF. The 2-year actuarial patient, kidney, and pancreas survival rates were 97.7%, 93.3%, and 90.0%, respectively. At 6 months after transplant, the overall incidence of acute rejection was 16%. There was a statistically significant (P< or =0.04, Cox-Mantel test) difference in the rate of rejection associated with conversion to Neoral. The incidence of rejection 6 months after transplant in the group maintained on MMF/tacrolimus was 10.2% vs. 44.4% in the group converted to Neoral (P< or =0.04, Cox-Mantel test). Overall, the 1-year actuarial cumulative incidence of tissue-invasive cytomegalovirus disease was 6.6%. There were no cases of fungal infections or post-transplant lymphoproliferative disorders. One patient developed Kaposi's sarcoma 10 months after transplant. With respect to hypertensive disease, 60% (12/20) of the patients who required pharmacologic control of blood pressure before transplant were off all antihypertensive medications at 1 year after transplant. An additional 20% (4/20) of patients had a reduction in the number of medications required to control blood pressure at 1 year after transplant.
We conclude that the combination of MMF and tacrolimus as primary immunosuppression for SPK transplantation results in excellent patient and graft survival rates, a very low rate of acute rejection, and low rates of infection and malignancy.
本研究探讨霉酚酸酯(MMF)和他克莫司作为同期胰肾联合移植(SPK)主要免疫抑制剂的应用情况。此外,还分析了从一种免疫抑制剂转换为另一种免疫抑制剂的发生率及其对移植结局的后续影响。同时描述了移植肾功能质量、感染情况以及对术前已存在的原发性高血压的影响。
免疫抑制采用抗胸腺细胞球蛋白诱导、他克莫司、MMF和泼尼松的四联疗法。描述了50例连续SPK受者的患者和移植物存活率及排斥反应发生率,随访时间至少3个月,平均14个月(范围:3 - 34个月)。
50例患者中有39例(78%)长期耐受MMF/他克莫司联合治疗(平均随访时间:14±7个月)。50例患者中有9例(18%)转换为新山地明,4例患者转换为硫唑嘌呤以替代MMF。患者、肾脏和胰腺的2年预期生存率分别为97.7%、93.3%和90.0%。移植后6个月时,急性排斥反应的总体发生率为16%。转换为新山地明后发生排斥反应的发生率存在统计学显著差异(P≤0.04,Cox - Mantel检验)。移植后6个月时,维持MMF/他克莫司治疗组的排斥反应发生率为10.2%,而转换为新山地明组为44.4%(P≤0.04,Cox - Mantel检验)。总体而言,组织侵袭性巨细胞病毒病的1年预期累积发生率为6.6%。未发生真菌感染或移植后淋巴细胞增生性疾病。1例患者在移植后10个月发生卡波西肉瘤。关于高血压疾病,移植前需要药物控制血压的患者中有60%(12/20)在移植后1年停用了所有抗高血压药物。另外20%(4/20)的患者在移植后1年控制血压所需的药物数量减少。
我们得出结论,MMF和他克莫司联合作为SPK移植的主要免疫抑制剂可带来优异的患者和移植物存活率、极低的急性排斥反应发生率以及低感染率和低恶性肿瘤发生率。
