Jurcic J G, Caron P C, Nikula T K, Papadopoulos E B, Finn R D, Gansow O A, Miller W H, Geerlings M W, Warrell R P, Larson S M
Leukemia Service, Memorial Sloan-Kettering Cancer Center, New York, New York 10021, USA.
Cancer Res. 1995 Dec 1;55(23 Suppl):5908s-5910s.
M195, a mouse monoclonal antibody reactive with the early myeloid antigen CD33, has been shown to target leukemia cells in patients and to reduce large leukemic burdens when labeled with 131I. A complementarity-determining region-grafted, humanized version (HuM195) has demonstrated similar targeting of leukemia cells without immunogenicity. We have studied two applications of therapy with 131I-M195. First, to intensify therapy prior to bone marrow transplantation (BMT), we combined 131I-M195 with busulfan and cyclophosphamide. Fifteen patients received first BMT for relapsed or refractory acute myelogenous leukemia or accelerated or blastic chronic myelogenous leukemia; four received second BMT for relapsed chronic or accelerated chronic myelogenous leukemia. Doses of 131I-M195 ranged from 120 to 230 mCi/m2. Few toxicities could be attributed to 131I-M195 therapy, and all patients engrafted. Eighteen patients achieved complete remission. Among those patients receiving first BMT, three have remained in unmaintained remission for 18+ to 29+ months. Six patients relapsed, including one with isolated central nervous system disease 32 months after BMT. Ten patients died in complete remission of transplant-related complications. Second, we studied whether 131I-M195 could reduce minimal residual disease and prolong remission and survival durations safely in patients with relapsed acute promyelocytic leukemia after they attained remission with all-trans-retinoic acid. Seven patients were treated with either 50 or 70 mCi/m2 131I-M195. Toxicity was limited to myelosuppression. As a measure of minimal residual disease, we monitored PML/RAR-alpha mRNA by reverse transcription PCR. Six patients had positive reverse transcription PCR assays prior to receiving 131I-M195; two converted transiently to negative. Median disease-free survival and overall survival of the seven patients were 8 (range, 3-14.5) months and 28 (range, 5.5-43+) months, respectively. This regimen compares favorably with others for relapsed acute promyelocytic leukemia. In an effort to avoid nonspecific cytotoxicity associated with 131I in future trials for minimal residual disease, we have conjugated short-range, alpha particle-emitting radioisotopes to HuM195 using a bifunctional chelate, 2-(p-isothiocyanatobenzyl)-cyclohexyldiethyl-enetriaminep entaacetic acid, with high efficiency and specific activities. 212Bi-HuM195 has demonstrated dose- and specific activity-dependent killing of HL60 cells in vitro. Injection of 213Bi-HuM195 into healthy BALB/c mice produced no effects on weight or viability.
M195是一种与早期髓系抗原CD33反应的小鼠单克隆抗体,已被证明可靶向患者体内的白血病细胞,并在用131I标记时减少大量白血病负荷。一种互补决定区移植的人源化版本(HuM195)已证明对白血病细胞具有类似的靶向作用且无免疫原性。我们研究了131I-M195治疗的两种应用。首先,为了在骨髓移植(BMT)前强化治疗,我们将131I-M195与白消安和环磷酰胺联合使用。15例患者因复发或难治性急性髓性白血病或加速期或急变期慢性髓性白血病接受首次BMT;4例因复发性慢性或加速期慢性髓性白血病接受第二次BMT。131I-M195的剂量范围为120至230 mCi/m2。很少有毒性可归因于131I-M195治疗,所有患者均成功植入。18例患者实现完全缓解。在接受首次BMT的患者中,3例在未维持缓解状态下分别持续了18 +至29 +个月。6例患者复发,其中1例在BMT后32个月出现孤立性中枢神经系统疾病。10例患者在完全缓解时死于移植相关并发症。其次,我们研究了131I-M195是否能在复发的急性早幼粒细胞白血病患者通过全反式维甲酸达到缓解后安全地减少微小残留病并延长缓解期和生存期。7例患者接受了50或70 mCi/m2的131I-M195治疗。毒性仅限于骨髓抑制。作为微小残留病的一项指标,我们通过逆转录聚合酶链反应监测PML/RAR-α mRNA。6例患者在接受131I-M195治疗前逆转录聚合酶链反应检测呈阳性;2例短暂转为阴性。这7例患者的无病生存期和总生存期的中位数分别为8(范围3 - 14.5)个月和28(范围5.5 - 43 +)个月。该方案与其他用于复发急性早幼粒细胞白血病的方案相比具有优势。为了在未来微小残留病试验中避免与131I相关的非特异性细胞毒性问题,我们使用双功能螯合剂2 -(对异硫氰酸苄基)-环己基二乙三胺五乙酸将发射短程α粒子的放射性同位素高效且高比活度地偶联到HuM195上。212Bi-HuM195已在体外证明对HL60细胞具有剂量和比活度依赖性杀伤作用。向健康的BALB/c小鼠注射213Bi-HuM195对体重或生存能力没有影响。
