Cremers Serge C L M, Papapoulos Socrates E, Gelderblom Hans, Seynaeve Caroline, den Hartigh Jan, Vermeij Pieter, van der Rijt Carin C D, van Zuylen Lia
Department of Clinical Pharmacy and Toxicology, Leiden University Medical Center, Leiden, The Netherlands.
J Bone Miner Res. 2005 Sep;20(9):1543-7. doi: 10.1359/JBMR.050522. Epub 2005 May 31.
Bisphosphonate pharmacokinetics may affect individual responses. Skeletal retention of pamidronate infused monthly to patients with bone metastases was highly variable (12-98%) and did not diminish with time, showing the capacity of the skeleton to retain large amounts of bisphosphonate. Relationships between skeletal retention of pamidronate and rate of bone resorption are complex and depend on previous treatment and the total amount of retained bisphosphonate.
Bisphosphonates (BPs) given intravenously every 3-4 weeks are effective in the management of metastatic bone disease from breast cancer, but responses among patients vary, and it is not known whether current dose and dose intervals are appropriate for an individual patient. An influence of pharmacokinetics of BPs on antiresorptive action may contribute to this variation in response. To test this hypothesis, we determined the skeletal retention of intravenous pamidronate and its association to the rate of bone resorption in patients with bone metastases from breast cancer.
In a cross-sectional study, 24-h urinary excretion of pamidronate and the biochemical marker of bone resorption N-terminal telopeptide of type 1 collagen and serum alkaline phosphatase were measured in 40 patients with bone metastases from breast cancer at the beginning, after 3-6 months, and after 1 year of treatment with intravenous pamidronate 90 mg every 3-4 weeks.
Skeletal retention (dose--amount excreted into urine) 2 days after infusion varied between 12% and 98% (mean, 62%) of the administered dose, but there were no differences in retention between patients receiving pamidronate for the first time or after 3-6 months or after 1 year of treatment. Retention of pamidronate was related to the prevalent rate of bone turnover in previously untreated patients, whereas no such relationship was found in previously treated patients. Rate of bone resorption after treatment seemed to be related to the amount of pamidronate retained. During 1 year of treatment, retention of pamidronate remained constant, indicating no saturation of skeletal binding sites with treatment. The variability in retention among individual patients can be attributed to the number of available binding sites. This is related, however, to bone turnover only before the start of treatment. The apparent relationships between skeletal retention and antiresorptive effect could have implications for the design of optimal therapeutic regimens with BPs in patients with bone metastases from breast cancer.
双膦酸盐的药代动力学可能会影响个体反应。每月给骨转移患者输注帕米膦酸后,其在骨骼中的保留率变化很大(12% - 98%),且不会随时间减少,这表明骨骼有保留大量双膦酸盐的能力。帕米膦酸在骨骼中的保留与骨吸收速率之间的关系很复杂,并且取决于先前的治疗情况以及保留的双膦酸盐总量。
每3 - 4周静脉注射一次双膦酸盐(BPs)对乳腺癌转移性骨病的治疗有效,但患者之间的反应存在差异,目前的剂量和给药间隔是否适合个体患者尚不清楚。双膦酸盐的药代动力学对抗吸收作用的影响可能是导致这种反应差异的原因。为了验证这一假设,我们测定了静脉注射帕米膦酸在乳腺癌骨转移患者骨骼中的保留情况及其与骨吸收速率的关系。
在一项横断面研究中,对40例乳腺癌骨转移患者在开始接受每3 - 4周静脉注射90 mg帕米膦酸治疗时、治疗3 - 6个月后以及治疗1年后,测定其24小时尿中帕米膦酸排泄量以及骨吸收生化标志物1型胶原N端前肽和血清碱性磷酸酶。
输注后2天骨骼保留量(剂量 - 尿中排泄量)在给药剂量的12%至98%之间(平均为62%),但首次接受帕米膦酸治疗的患者、治疗3 - 6个月后的患者以及治疗1年后的患者之间的保留量没有差异。帕米膦酸的保留与未接受过治疗患者中普遍的骨转换率有关,而在先前接受过治疗的患者中未发现这种关系。治疗后的骨吸收速率似乎与保留的帕米膦酸量有关。在1年的治疗期间,帕米膦酸的保留量保持恒定,表明治疗并未使骨骼结合位点饱和。个体患者之间保留量的差异可归因于可用结合位点的数量。然而,这仅与治疗开始前的骨转换有关。骨骼保留与抗吸收作用之间的明显关系可能对乳腺癌骨转移患者双膦酸盐最佳治疗方案的设计具有启示意义。
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