Cox Victoria C, Ensom Mary H H
Faculty of Pharmaceutical Sciences, University of British Columbia, Vancouver, British Columbia, Canada.
Ther Drug Monit. 2003 Apr;25(2):137-57. doi: 10.1097/00007691-200304000-00003.
The need for clinical pharmacokinetic monitoring (CPM) of the immunosuppressant mycophenolate mofetil (MMF) has been debated. Using a previously developed algorithm, the authors reviewed the evidence to support or refute the utility of CPM of MMF. First, MMF has proven efficacy for prevention of organ rejection in renal and cardiac transplant populations. In addition, the pharmacologically active form of MMF, mycophenolic acid (MPA), can be measured readily in plasma, and relationships between the incidence of rejection and MPA predose concentrations and MPA area under the curve (AUC) have been reported. A lower limit of the therapeutic range (MPA predose concentrations >1.55 microg/mL, as measured by enzyme multiplied immunoassay technique [EMIT], or MPA AUC >30 or 40 microg. h/mL, as measured by high-performance liquid chromatography [HPLC]) has been suggested to prevent rejection in renal allograft patients. Similarly, in cardiac transplant patients, decreased incidences of organ rejection have been reported in patients with MPA concentrations >2 or 3 microg/mL (using EMIT) and total AUC values >42.8 microg. h/mL (using HPLC). However, the relationship between pharmacokinetic parameters and adverse events in renal and cardiac transplant patients remains unclear. Due to the nature of antirejection therapy, the pharmacologic response of MMF is not readily assessable, and therapy is life-long. MPA pharmacokinetics exhibit large inter- and intrapatient variability and may be altered in specific patient populations due to changes in protein binding, concomitant disease states, or interactions with concurrent immunosuppressants. Therefore, on the basis of current evidence, CPM can provide more information regarding efficacy of MMF than clinical judgment alone in select patient populations. However, further randomized, prospective trials are required to clarify unresolved issues. Specifically, an upper limit of the therapeutic range, above which the risk of side effects is increased, needs to be elucidated for MMF therapy. Other future directions for research include determining a practical limited sampling strategy for MPA AUC; clarifying the relationship between free MPA concentrations, efficacy, and toxicity; and defining the pharmacodynamic relationship between activity of inosine monophosphate dehydrogenase (the enzyme inhibited by MPA) and risk of rejection or adverse effects.
免疫抑制剂霉酚酸酯(MMF)的临床药代动力学监测(CPM)的必要性一直存在争议。作者使用先前开发的算法,回顾了支持或反驳MMF的CPM效用的证据。首先,MMF已被证明在肾移植和心脏移植人群中预防器官排斥反应有效。此外,MMF的药理活性形式霉酚酸(MPA)可在血浆中轻松测量,并且已经报道了排斥反应发生率与MPA给药前浓度以及MPA曲线下面积(AUC)之间的关系。有人建议治疗范围下限(通过酶放大免疫分析技术[EMIT]测量,MPA给药前浓度>1.55μg/mL,或通过高效液相色谱法[HPLC]测量,MPA AUC>30或40μg·h/mL)可预防肾移植患者发生排斥反应。同样,在心脏移植患者中,据报道MPA浓度>2或3μg/mL(使用EMIT)且总AUC值>42.8μg·h/mL(使用HPLC)的患者器官排斥反应发生率降低。然而,肾移植和心脏移植患者的药代动力学参数与不良事件之间的关系仍不清楚。由于抗排斥治疗的性质,MMF的药理反应不易评估,且治疗是终身的。MPA药代动力学在患者间和患者内表现出很大的变异性,并且由于蛋白质结合、伴随疾病状态或与同时使用的免疫抑制剂相互作用的变化,在特定患者群体中可能会改变。因此,根据目前的证据,在特定患者群体中,CPM比单独的临床判断可以提供更多关于MMF疗效的信息。然而,需要进一步的随机前瞻性试验来澄清未解决的问题。具体而言,需要阐明MMF治疗的治疗范围上限,超过该上限副作用风险会增加。未来其他研究方向包括确定MPA AUC的实用有限采样策略;阐明游离MPA浓度、疗效和毒性之间的关系;以及确定肌苷单磷酸脱氢酶(被MPA抑制的酶)活性与排斥反应风险或不良反应之间的药效学关系。
