Mazziotti Gherardo, Rodari Marcello, Gelardi Fabrizia, Tosi Giovanni, Zucali Paolo A, Pepe Giovanna, Chiti Arturo
Endocrinology, Diabetology and Andrology Unit, Metabolic Bone Diseases and Osteoporosis Section, Humanitas Clinical and Research Center, IRCCS, Milan, Italy.
Department of Biomedical Sciences, Humanitas University, Milan, Italy.
Endocrine. 2020 Jul;69(1):204-211. doi: 10.1007/s12020-020-02277-6. Epub 2020 Apr 1.
Radium-223 was associated with high incidence of non-vertebral fractures in patients with castration-resistant prostate cancer (CRPC). However, it is still unclear whether radium-223 may induce skeletal fragility regardless of other therapies for CRPC. We aimed at evaluating the prevalence, incidence, and determinants of vertebral fractures (VFs), i.e., the most frequent complication of skeletal fragility, in CRCP patients undergoing radium-223 therapy in the real-life clinical practice.
We retrospectively reviewed 49 CRPC patients with symptomatic bone metastases treated with radium-223. Patients received median number of four radium-223 doses (range: 2-6) and were followed-up for a median period of 11 months (range: 6-44). VFs were assessed by a quantitative morphometry using lateral images of spine 11C-Choline PET/CT, excluding from the analysis the vertebral bodies affected by bone metastases.
Before radium-223 administration, 24 patients (49%) had VFs significantly associated with duration of androgen deprivation therapy (ADT; odds ratio 1.29) and previous abiraterone therapy (odds ratio 3.80). During radium-223 therapy, incident VFs occurred in 25% of patients, in relationship with prevalent VFs (hazard ratio 6.89) and change in serum total alkaline phosphatase values (hazard ratio 0.97), whereas the correlations with ADT and abiraterone therapy were lost. Noteworthy, the risk of VFs did not correlate with the therapeutic end points of radium-223.
This study provides a first evidence that in real-life clinical practice, radium-223 therapy may induce skeletal fragility with high risk of VFs, likely by inhibition of bone formation and independently of ADT and abiraterone therapy.
镭-223与去势抵抗性前列腺癌(CRPC)患者非椎体骨折的高发生率相关。然而,镭-223是否会导致骨骼脆弱,而不考虑CRPC的其他治疗方法,目前仍不清楚。我们旨在评估在实际临床实践中接受镭-223治疗的CRCP患者中椎体骨折(VFs)的患病率、发生率及相关因素,VFs是骨骼脆弱最常见的并发症。
我们回顾性分析了49例接受镭-223治疗的有症状骨转移的CRPC患者。患者接受的镭-223剂量中位数为4次(范围:2 - 6次),中位随访时间为11个月(范围:6 - 44个月)。通过使用脊柱11C - 胆碱PET/CT的侧位图像进行定量形态学评估VFs,分析时排除受骨转移影响的椎体。
在给予镭-223之前,24例患者(49%)存在VFs,这与雄激素剥夺治疗(ADT)的持续时间(比值比1.29)和既往阿比特龙治疗(比值比3.80)显著相关。在镭-223治疗期间,25%的患者发生新发VFs,与既往存在的VFs(风险比6.89)和血清总碱性磷酸酶值的变化(风险比0.97)有关,而与ADT和阿比特龙治疗的相关性消失。值得注意的是,VFs的风险与镭-223的治疗终点无关。
本研究首次证明在实际临床实践中,镭-223治疗可能导致骨骼脆弱并伴有高VFs风险,可能是通过抑制骨形成,且独立于ADT和阿比特龙治疗。
