Weber G, Jayaram H N, Lapis E, Natsumeda Y, Yamada Y, Yamaji Y, Tricot G J, Hoffman R
Laboratory for Experimental Oncology, Indiana University School of Medicine, Indianapolis 46223.
Adv Enzyme Regul. 1988;27:405-33. doi: 10.1016/0065-2571(88)90029-5.
The hypothesis was tested that the increased IMP dehydrogenase activity in human myelocytic leukemic cells, and along with it guanylate biosynthesis, might be a sensitive target to chemotherapy by tiazofurin. 1. IMP dehydrogenase activity in normal leukocytes was 3.1 +/- 0.5 (means +/- S.E.) nmol/hr/mg protein and in leukemic cells it was elevated 15- to 41-fold. The activity of guanine phosphoribosyltransferase in normal leukocytes was 389 +/- 27 nmol/hr/mg protein and in the leukemic cells it increased 2.8- to 6.8-fold. 2. IMP dehydrogenase was purified 4,900-fold to homogeneity from rat hepatoma 3924A with a yield of 30%. The kinetic properties of the hepatoma enzyme were similar to those of the enzyme in human myelocytic leukemic blast cells because of the similarity of the Km's for IMP (23 microM), NAD (44 and 65 microM); the Ki for TAD was 0.1 microM in both enzymes. 3. There was a selectivity of the in vitro response to tiazofurin in human normal and leukemic leukocytes. When labeled tiazofurin was incubated with leukocytes from normal, healthy volunteers and from leukemic patients, the leukemic leukocytes made 20- to 30-fold more TAD and the GTP content decreased as compared to normal leukocytes. This procedure proved to be a suitable predictive test in a clinical setting because patients with positive tests responded to tiazofurin whereas those with negative ones did not. 4. The National Cancer Institute approved a chemotherapeutic phase I/II trial which concentrates on treatment of refractory acute myelocytic leukemia. Tiazofurin is infused in a 60-minute period with a pump to insure uniform delivery. A novel aspect of the trial was that it was directed primarily by the biochemical impact of tiazofurin on IMP dehydrogenase activity and GTP concentration and the tiazofurin doses were to be adjusted accordingly. Patients received allopurinol as a routine precaution against possible accumulation of uric acid in the kidney. 5. In the first eight patients, there was one complete remission, two entered the chronic phase, two entered into partial remission, one did not respond, and two were not evaluable. In the five patients who responded, there was a rapid, profound decrease in IMP dehydrogenase activity of the blast cells and a gradual decline in GTP concentrations. The blast cell count followed the decrease in the GTP concentration. The white blood cell count was largely preserved. 6. Bone marrow aspirates and peripheral blood samples showed that with tiazofurin treatment there was an induced differentiation of the myelocytes.(ABSTRACT TRUNCATED AT 400 WORDS)
有一个假说得到了验证,即人类髓细胞白血病细胞中 IMP 脱氢酶活性的增加以及与之相伴的鸟苷酸生物合成,可能是替加氟尿嘧啶化疗的一个敏感靶点。1. 正常白细胞中的 IMP 脱氢酶活性为 3.1±0.5(均值±标准误)nmol/小时/毫克蛋白,而白血病细胞中的该活性升高了 15 至 41 倍。正常白细胞中鸟嘌呤磷酸核糖转移酶的活性为 389±27 nmol/小时/毫克蛋白,白血病细胞中的该活性增加了 2.8 至 6.8 倍。2. 从大鼠肝癌 3924A 中纯化出的 IMP 脱氢酶达到了 4900 倍的纯度且具有同质性,产率为 30%。肝癌酶的动力学特性与人类髓细胞白血病原始细胞中的酶相似,因为两者对 IMP(23μM)、NAD(44 和 65μM)的 Km 值相似;两种酶对 TAD 的 Ki 值均为 0.1μM。3. 人类正常和白血病白细胞对替加氟尿嘧啶的体外反应具有选择性。当用标记的替加氟尿嘧啶与正常健康志愿者和白血病患者的白细胞一起孵育时,与正常白细胞相比,白血病白细胞产生的 TAD 多 20 至 30 倍,且 GTP 含量降低。该程序在临床环境中被证明是一种合适的预测性检测方法,因为检测呈阳性的患者对替加氟尿嘧啶有反应,而检测呈阴性的患者则无反应。4. 美国国立癌症研究所批准了一项化疗 I/II 期试验,该试验主要针对难治性急性髓细胞白血病的治疗。用泵在 60 分钟内输注替加氟尿嘧啶以确保均匀给药。该试验的一个新特点是,它主要由替加氟尿嘧啶对 IMP 脱氢酶活性和 GTP 浓度的生化影响来指导,并且替加氟尿嘧啶的剂量将相应调整。患者常规服用别嘌呤醇以预防肾脏中尿酸可能的蓄积。5. 在前八名患者中,有一名完全缓解,两名进入慢性期,两名进入部分缓解期,一名无反应,两名无法评估。在有反应的五名患者中,原始细胞的 IMP 脱氢酶活性迅速、显著下降,GTP 浓度逐渐降低。原始细胞计数随 GTP 浓度的降低而下降。白细胞计数基本保持不变。6. 骨髓穿刺液和外周血样本显示,用替加氟尿嘧啶治疗可诱导髓细胞分化。(摘要截短至 400 字)
