Schroeder T J, First M R, Mansour M E, Hurtubise P E, Hariharan S, Ryckman F C, Munda R, Melvin D B, Penn I, Ballistreri W F
Department of Pathology and Laboratory Medicine, University of Cincinnati, OH 45267-0714.
Transplantation. 1990 Jan;49(1):48-51. doi: 10.1097/00007890-199001000-00010.
OKT3 is an IgG2a murine monoclonal antibody directed against the CD3 antigen receptor of human T lymphocytes. A major concern with OKT3 treatment in solid organ transplant recipients is the development of antimouse antibody, which may preclude retreatment with this agent. We have administered OKT3 on 215 occasions (150 renal, 34 hepatic, 26 cardiac, 5 pancreatic) in 179 patients between April 1982 and December 1988. The mean duration of treatment was 10.5 days (range, 2-22 days). Antimouse antibody data were analyzed on the most recent 133 treatment courses where the antibody status was available pretreatment. Determination of antimouse antibody production was elicited by ELISA technology at days 0, 7, 14, and 28 of OKT3 treatment. Patients were categorized according to the antibody response as follows: (a) absence of antibody; (b) low titer (1:100); or (c) high titer (greater than or equal to 1:1000). Our earlier experience has demonstrated that retreatment with OKT3 is successful in groups a and b. The development of antimurine antibodies was analyzed with regard to the following parameters: (1) The duration of OKT3 treatment; (2) treatment type (prophylactic, primary, or secondary); (3) primary treatment or retreatment; (4) concomitant immunosuppressive regimen (double or triple therapy); (5) dosage of concomitant immunosuppressive drugs; and (6) transplant organ type. The following results were obtained. (1) Duration of treatment had no effect on antibody production (11.0 days in antibody negative and 10.0 days in antibody positive). (2) There was no difference in antibody formation rates for the first treatment of OKT3 when it was used as prophylaxis (26%), primary (19%), or secondary (27%) therapy. (3) Antibody formation rate with first treatment was 29%; with retreatment, patients who were antibody negative following first treatment became positive in 28% of cases, and retreated patients who were low titer positive following first treatment converted to high titer in 57% of cases. (4) Antibody formation was higher in patients receiving double immunosuppressive therapy (36%) than in those receiving triple immunosuppressive therapy (21%) during OKT3 treatment. (5) Concomitant immunosuppression was lower in the antibody-positive group during OKT3 therapy: steroids, 61 mg/day vs. 52 mg/day; azathioprine, 89 mg/day vs. 66 mg/day; CsA, 317 mg/day vs. 186 mg/day. (6) Antibody formation rates were lower in non-renal transplants following first treatment with OKT3 (liver 17%, heart 17%, kidney 28%); this reflects the higher doses of concomitant immunosuppressive therapy used in nonrenal transplants.(ABSTRACT TRUNCATED AT 400 WORDS)
OKT3是一种针对人T淋巴细胞CD3抗原受体的IgG2a鼠单克隆抗体。实体器官移植受者接受OKT3治疗的一个主要问题是抗鼠抗体的产生,这可能会妨碍再次使用该药物进行治疗。1982年4月至1988年12月期间,我们对179例患者进行了215次OKT3给药(150例肾脏移植、34例肝脏移植、26例心脏移植、5例胰腺移植)。平均治疗持续时间为10.5天(范围为2 - 22天)。对最近133个治疗疗程中可获得预处理抗体状态的抗鼠抗体数据进行了分析。在OKT3治疗的第0、7、14和28天,通过ELISA技术检测抗鼠抗体的产生情况。根据抗体反应将患者分为以下几类:(a)无抗体;(b)低滴度(1:100);或(c)高滴度(大于或等于1:1000)。我们早期的经验表明,对a组和b组患者再次使用OKT3治疗是成功的。针对以下参数分析了抗鼠抗体的产生情况:(1)OKT3治疗持续时间;(2)治疗类型(预防性、初次或二次治疗);(3)初次治疗或再次治疗;(4)联合免疫抑制方案(双重或三重治疗);(5)联合免疫抑制药物剂量;以及(6)移植器官类型。获得了以下结果。(1)治疗持续时间对抗体产生无影响(抗体阴性组为11.0天,抗体阳性组为10.0天)。(2)OKT3首次用作预防性治疗(26%)、初次治疗(19%)或二次治疗(27%)时,抗体形成率无差异。(3)首次治疗时抗体形成率为29%;再次治疗时,首次治疗后抗体阴性的患者中有28%转为阳性,首次治疗后低滴度阳性的再次治疗患者中有57%转为高滴度。(4)在OKT3治疗期间,接受双重免疫抑制治疗的患者(36%)的抗体形成率高于接受三重免疫抑制治疗的患者(21%)。(5)OKT3治疗期间,抗体阳性组的联合免疫抑制水平较低:类固醇,61毫克/天对52毫克/天;硫唑嘌呤,89毫克/天对66毫克/天;环孢素A,317毫克/天对186毫克/天。(6)OKT3首次治疗后,非肾脏移植患者的抗体形成率较低(肝脏17%,心脏17%,肾脏28%);这反映了非肾脏移植中使用的联合免疫抑制治疗剂量较高。(摘要截短至400字)
