Hausen B, Gummert J, Berry G J, Christians U, Serkova N, Ikonen T, Hook L, Legay F, Schuler W, Schreier M H, Morris R E
Transplantation Immunology, Department of Cardiothoracic Surgery, Stanford University, Palo Alto, California 94305, USA.
Transplantation. 2000 Feb 27;69(4):488-96. doi: 10.1097/00007890-200002270-00005.
In previous studies of cynomolgus monkey lung allograft recipients, we demonstrated significant immunosuppressive efficacy but reduced tolerability after combined treatment with high doses of microemulsion cyclosporine (CsA) and SDZ RAD (40-O-(2-hydroxyethyl)-rapamycin). The current study was designed to compare efficacy and tolerability of a combination of low-dose CsA and high-dose SDZ RAD (CTL group) to triple therapy using the chimeric anti-interleukin-2 (IL-2) receptor (CD25) monoclonal antibody (mAb) basiliximab (anti-IL-2 receptor mAb) for induction therapy (basiliximab: 5 mg intravenously on days 0 and 4) plus low-dose CsA and low-dose SDZ RAD for maintenance immunosuppression (CD25 group). CsA and anti-IL-2 receptor mAb are drugs that reduce cytokine synthesis and block IL-2-mediated lymphocyte stimulation, respectively. SDZ RAD blocks lymphocyte stimulation by other cytokines (e.g., IL-15) that are not inhibited by anti-IL-2 receptor mAb.
Twelve unilateral lung transplants were performed. Recipients were observed for 49 days by daily weight assessment, hemograms, blood chemistries, radiographs, and lung biopsies. Monkeys were euthanized before day 49 in the event of excessive weight loss (>25%) or organ failure. Target CsA trough levels were 100-200 ng/ml. Target SDZ RAD trough levels in the CTL group (no mAb) were 20-40 ng/ml, and 10-20 ng/ml in the CD25 group.
None of the monkeys in the CD25 group needed to be euthanized early due to signs of drug toxicity. In contrast, four monkeys in the CTL group were sacrificed on days 28-35 as a result of excessive weight loss (n=3) and renal functional impairment (n=1). Three recipients in the CD25 group were euthanized on days 36, 38, and 46 as a result of persistent high fever associated with severe rejection. The median animal survival in the CTL group was 32 vs. 46 days in the CD25 group (P<0.04). The only two long-term survivors in the CTL group showed moderate rejection at day 49. The median rejection scores at day 14 (A0) and day 28 (A2) were identical in the two groups, despite the fact that the mean SDZ RAD trough level was significantly lower in the CD25 group (CTL: 38+/-3 ng/ml, CD25: 18+/-2 ng/ml, P<0.0001). After basiliximab levels fell below the minimum therapeutic level (1 mg/ml) on day 28, the median rejection score at day 49 increased to A4 in the CD25 group.
This is the first study to combine an anti-IL-2 receptor mAb with a drug from the rapamycin class plus CsA. Our study shows that induction therapy with basiliximab enabled SDZ RAD blood levels to be significantly reduced, which led to improved tolerability without the penalty of increased rejection.
在之前对食蟹猴肺移植受者的研究中,我们证明了高剂量微乳环孢素(CsA)和SDZ RAD(40 - O -(2 - 羟乙基)-雷帕霉素)联合治疗具有显著的免疫抑制效果,但耐受性降低。本研究旨在比较低剂量CsA与高剂量SDZ RAD联合治疗组(CTL组)和使用嵌合抗白细胞介素 - 2(IL - 2)受体(CD25)单克隆抗体(mAb)巴利昔单抗进行诱导治疗(巴利昔单抗:在第0天和第4天静脉注射5 mg)加低剂量CsA和低剂量SDZ RAD进行维持免疫抑制的三联疗法组(CD25组)的疗效和耐受性。CsA和抗IL - 2受体mAb分别是减少细胞因子合成和阻断IL - 2介导的淋巴细胞刺激的药物。SDZ RAD可阻断其他细胞因子(如IL - 15)介导的淋巴细胞刺激,而这些细胞因子不会被抗IL - 2受体mAb抑制。
进行了12例单侧肺移植。通过每日体重评估、血常规、血液化学检查、X光片和肺活检对受者进行49天的观察。若体重过度减轻(>25%)或出现器官衰竭,则在第49天之前对猴子实施安乐死。目标CsA谷浓度为100 - 200 ng/ml。CTL组(无mAb)的目标SDZ RAD谷浓度为20 - 40 ng/ml,CD25组为10 - 20 ng/ml。
CD25组中没有猴子因药物毒性迹象而需要提前实施安乐死。相比之下,CTL组中有4只猴子在第28 - 35天因体重过度减轻(n = 3)和肾功能损害(n = 1)而被处死。CD25组中有3只受者因与严重排斥相关的持续高热在第36、38和46天被安乐死。CTL组的动物中位生存时间为32天,而CD25组为46天(P < 0.04)。CTL组仅有的两名长期存活者在第49天显示出中度排斥。尽管CD25组的平均SDZ RAD谷浓度显著低于CTL组(CTL:38 ± 3 ng/ml,CD25:18 ± 2 ng/ml,P < 0.0001),但两组在第14天(A0)和第28天(A2)的中位排斥评分相同。在第28天巴利昔单抗水平降至最低治疗水平(1 mg/ml)以下后,CD25组在第49天的中位排斥评分增加至A4。
这是第一项将抗IL - 2受体mAb与雷帕霉素类药物加CsA联合使用的研究。我们的研究表明,巴利昔单抗诱导治疗能够显著降低SDZ RAD的血药浓度,从而提高耐受性,且不会增加排斥反应。
