Coukell A J, Markham A
Adis International Limited, Auckland, New Zealand.
Drugs Aging. 1998 Feb;12(2):149-68. doi: 10.2165/00002512-199812020-00007.
Pamidronate (APD) is a potent inhibitor of bone resorption that is useful in the management of patients with osteolytic bone metastases from breast cancer or multiple myeloma, tumour-induced hypercalcaemia or Paget's disease of bone. After intravenous administration, the drug is extensively taken up in bone, where it binds with hydroxyapatite crystals in the bone matrix. Matrix-bound pamidronate inhibits osteoclast activity by a variety of mechanisms, the most important of which appears to be prevention of the attachment of osteoclast precursor cells to bone. In patients with osteolytic bone metastases associated with either breast cancer or multiple myeloma, administration of pamidronate together with systemic antitumour therapy reduces and delays skeletal events, including pathological fracture, hypercalcaemia and the requirement for radiation treatment or surgery to bone. Pamidronate generally improves pain control. Quality-of-life and performance status scores in pamidronate recipients were generally as good as, or better than, those in patients who did not receive the drug. Overall survival does not appear to be affected by pamidronate therapy. Tumour-induced hypercalcaemia also responds well to pamidronate therapy: 70 to 100% of patients achieve normocalcaemia, generally 3 to 5 days after treatment. Response durations vary, but are commonly 3 weeks or longer, In comparative studies, pamidronate produced higher rates of normocalcaemia and longer normocalcaemic durations than other available osteoclast inhibitors, including intravenous etidronate, clodronate and plicamycin (mithramycin). In most patients with Paget's disease of bone, intravenous pamidronate reduces bone pain and produces biochemical response. Serum alkaline phosphatase levels generally fall 50 to 70% from baseline 3 to 4 months after pamidronate treatment. Biochemical response may be prolonged. Pamidronate is well tolerated by most patients. Transient febrile reactions, sometimes accompanied by myalgias and lymphopenia, occur commonly after the first infusion of pamidronate. Other reported adverse events include transient neutropenia, mild thrombophlebitis, asymptomatic hypocalcaemia and, rarely, ocular complications (uveitis and scleritis). Pamidronate should be considered for routine use together with systemic hormonal or cytotoxic therapy in patients with breast cancer or multiple myeloma and osteolytic metastases. At present, pamidronate is the drug of choice for first-line use in the management of patients with tumour-induced hypercalcaemia. It is an effective treatment for Paget's disease and is the treatment of choice where oral bisphosphonates are not an option.
帕米膦酸盐(APD)是一种强效的骨吸收抑制剂,可用于治疗乳腺癌或多发性骨髓瘤引起的溶骨性骨转移、肿瘤诱导的高钙血症或佩吉特骨病患者。静脉给药后,该药物在骨骼中被大量摄取,并与骨基质中的羟基磷灰石晶体结合。与骨基质结合的帕米膦酸盐通过多种机制抑制破骨细胞活性,其中最重要的机制似乎是阻止破骨细胞前体细胞附着于骨。在患有与乳腺癌或多发性骨髓瘤相关的溶骨性骨转移患者中,将帕米膦酸盐与全身抗肿瘤治疗联合使用可减少并延迟骨骼事件,包括病理性骨折、高钙血症以及对骨骼进行放射治疗或手术的需求。帕米膦酸盐通常可改善疼痛控制。接受帕米膦酸盐治疗的患者的生活质量和功能状态评分通常与未接受该药物治疗的患者相同或更好。总体生存率似乎不受帕米膦酸盐治疗的影响。肿瘤诱导的高钙血症对帕米膦酸盐治疗也有良好反应:70%至100%的患者血钙恢复正常,通常在治疗后3至5天。反应持续时间各不相同,但通常为3周或更长时间。在比较研究中,与其他可用的破骨细胞抑制剂(包括静脉注射依替膦酸盐、氯膦酸盐和普卡霉素(光辉霉素))相比,帕米膦酸盐产生正常血钙水平的比例更高,正常血钙持续时间更长。在大多数佩吉特骨病患者中,静脉注射帕米膦酸盐可减轻骨痛并产生生化反应。帕米膦酸盐治疗后3至4个月,血清碱性磷酸酶水平通常较基线下降50%至70%。生化反应可能会延长。大多数患者对帕米膦酸盐耐受性良好。首次输注帕米膦酸盐后通常会出现短暂的发热反应,有时伴有肌痛和淋巴细胞减少。其他报告的不良事件包括短暂性中性粒细胞减少、轻度血栓性静脉炎、无症状性低钙血症,以及罕见的眼部并发症(葡萄膜炎和巩膜炎)。对于患有乳腺癌或多发性骨髓瘤及溶骨性转移的患者,应考虑将帕米膦酸盐与全身激素或细胞毒性治疗联合常规使用。目前,帕米膦酸盐是治疗肿瘤诱导的高钙血症患者一线使用的首选药物。它是佩吉特骨病的有效治疗方法,也是口服双膦酸盐不可行时的首选治疗方法。
