Body J J, Lortholary A, Romieu G, Vigneron A M, Ford J
Supportive Care Clinic & Bone Diseases Clinic, Institut J. Bordet, Université Libre de Bruxelles, Brussels, Belgium.
J Bone Miner Res. 1999 Sep;14(9):1557-61. doi: 10.1359/jbmr.1999.14.9.1557.
Zoledronate is a new heterocyclic imidazole bisphosphonate that is the most potent bisphosphonate administered in humans because it is 100-850 times more potent than pamidronate, according to in vitro or animal models of bone resorption. We conducted an open-label, dose-finding, single-dose phase I study in tumor-induced hypercalcemia (TIH), which has been similarly used as a model to determine the active doses of other bisphosphonates. The primary objective was to determine, with a dose escalation schedule, two nontoxic dose levels of zoledronate able to induce normocalcemia in at least 80% of patients with TIH after rehydration (corrected Ca for albumin levels >/=2.75 mmol/l). Based on estimates of potency, the starting dose was 0.002 mg/kg, and further tested doses were 0. 005, 0.01, 0.02, and 0.04 mg/kg. To obtain a more precise estimate of the response rate, we treated 10 more patients at the highest of the two effective dose levels. The median infusion time of zoledronate was 30 minutes. Thirty out of the 33 treated patients were evaluable for efficacy. Thirty percent of the patients had breast cancer and 54% had metastatic bone involvement. For all groups combined, mean Ca levels at baseline was 3.0 mmol/l. The two effective dose levels were 0.02 mg/kg and 0.04 mg/kg. Five out of five patients became normocalcemic after 0.02 mg of zoledronate/kg and 14 out of 15 after 0.04 mg of zoledronate/kg. The success rate of the latter dose was thus 93% (95% confidence interval [CI] 68-100%). At this dose, the first day of normocalcemia was day 2 or 3 for all but one patient. The duration of normocalcemia for the two effective doses could be assessed in nine patients; seven patients remained normocalcemic throughout the trial (32-39 days). The fall in serum Ca was accompanied by a marked fall in fasting urinary Ca excretion. Zoledronate was well tolerated: 7 out of 33 patients developed transient hypophosphatemia, and 3 developed transient hypocalcemia. The only clinically detectable side effect was an increase in body temperature occurring in 10 (30%) patients. In summary, very low doses of zoledronate (0.02 mg/kg and 0.04 mg/kg, i. e., 1.2 mg and 2.4 mg for a 60-kg individual, respectively) administered by a short-time infusion effectively treated patients with TIH. The fall in serum Ca was rapid, and normocalcemia was often maintained for several weeks. Zoledronate was well tolerated. Future trials will determine whether prolonged treatment with this potent compound can have greater effects on the skeletal morbidity rate in patients with tumor bone disease than can be achieved with currently available bisphosphonates.
唑来膦酸盐是一种新型杂环咪唑双膦酸盐,根据体外或骨吸收动物模型,它是在人体中使用的最有效的双膦酸盐,其效力比帕米膦酸盐高100 - 850倍。我们对肿瘤诱导的高钙血症(TIH)进行了一项开放标签、剂量探索、单剂量I期研究,TIH同样被用作确定其他双膦酸盐活性剂量的模型。主要目的是通过剂量递增方案确定两个无毒剂量水平的唑来膦酸盐,在补液后(白蛋白水平校正钙≥2.75 mmol/l)至少80%的TIH患者中能够诱导血钙正常。基于效力估计,起始剂量为0.002 mg/kg,进一步测试的剂量为0.005、0.01、0.02和0.04 mg/kg。为了更精确地估计反应率,我们在两个有效剂量水平中最高的那个剂量水平上又治疗了10名患者。唑来膦酸盐的中位输注时间为30分钟。33名接受治疗的患者中有30名可进行疗效评估。30%的患者患有乳腺癌,54%有骨转移。所有组合并后,基线时的平均钙水平为3.0 mmol/l。两个有效剂量水平为0.02 mg/kg和0.04 mg/kg。0.02 mg唑来膦酸盐/kg后5名患者中有5名血钙恢复正常,0.04 mg唑来膦酸盐/kg后15名患者中有14名恢复正常。因此,后一个剂量的成功率为93%(95%置信区间[CI] 68 - 100%)。在此剂量下,除一名患者外,所有患者血钙正常的第一天为第2天或第3天。可以在9名患者中评估两个有效剂量的血钙正常持续时间;7名患者在整个试验期间(32 - 39天)保持血钙正常。血清钙下降伴随着空腹尿钙排泄的显著下降。唑来膦酸盐耐受性良好:33名患者中有7名出现短暂性低磷血症,3名出现短暂性低钙血症。唯一临床可检测到的副作用是10名(30%)患者体温升高。总之,通过短时间输注给予非常低剂量的唑来膦酸盐(0.02 mg/kg和0.04 mg/kg,即60 kg个体分别为1.2 mg和2.4 mg)可有效治疗TIH患者。血清钙下降迅速,血钙正常通常维持数周。唑来膦酸盐耐受性良好。未来的试验将确定用这种强效化合物进行长期治疗是否对肿瘤骨病患者的骨骼发病率有比目前可用的双膦酸盐更大的影响。
