用于接受雄激素剥夺治疗的前列腺癌患者骨质流失的骨改良剂;网状Meta分析的见解
Bone-modifying agents for bone loss in patients with prostate cancer receiving androgen deprivation therapy; insights from a network meta-analysis.
作者信息
Miyashita Hirotaka, Satoi Sera, Cruz Christina, Kim Se-Min, Patel Vaibhav G
机构信息
Department of Medicine, Icahn School of Medicine At Mount Sinai, Mount Sinai Beth Israel, New York, NY, USA.
Mount Sinai Bone Program, Icahn School of Medicine At Mount Sinai, New York, NY, USA.
出版信息
Support Care Cancer. 2022 Jan;30(1):855-863. doi: 10.1007/s00520-021-06490-5. Epub 2021 Aug 15.
BACKGROUND
The data of head-to-head comparisons of the effect of bone-modifying agents (BMAs) in patients with androgen deprivation therapy (ADT) for prostate cancer without skeletal metastasis is limited. Thus, we conducted a network meta-analysis to compare each BMA for the efficacy of bone mineral densities (BMDs) and the risk of fracture.
METHODS
We performed a network meta-analysis to compare the change of BMDs and the risk of vertebral fracture in the studies included using a random-effect model. The primary outcomes are the change of BMD of the lumbar spine (LS) and the total hip (TH) from the baseline at 1 year from the initiation of the BMA and the risk of vertebral fracture.
RESULTS
We identified and included 15 studies in this analysis. All BMAs except risedronate showed a significant increase of BMD of the LS compared with groups without BMA, among which zoledronate showed the most BMD gain. At TH, bisphosphonates (alendronate, pamidronate, and zoledronate) and denosumab showed significant elevation compared with the no-BMA group. Denosumab was associated with the most BMD gain at the TH. Only denosumab reduced the risk of vertebral fracture (relative risk [95% confidence interval]: 0.40 [0.20-0.81]). Although zoledronate showed the highest BMD gain at the LS, it did not reduce the risk of vertebral fracture in this analysis.
CONCLUSION
Most bisphosphonates and denosumab significantly increased BMD at the LS and the TH in patients receiving ADT for prostate cancer without skeletal metastasis. In particular, zoledronate and denosumab were the most potent BMAs in terms of BMD increment at the LS and the TH, respectively. However, denosumab, not zoledronate, was the only BMA that showed a significant risk reduction of vertebral fracture. We need further studies to examine the change of bone quality and the effect on the risk of non-vertebral and hip fractures.
背景
在没有骨转移的前列腺癌雄激素剥夺治疗(ADT)患者中,骨改良剂(BMA)疗效的头对头比较数据有限。因此,我们进行了一项网状Meta分析,以比较每种BMA在骨矿物质密度(BMD)和骨折风险方面的疗效。
方法
我们进行了一项网状Meta分析,以使用随机效应模型比较纳入研究中BMD的变化和椎体骨折风险。主要结局是从开始使用BMA起1年时腰椎(LS)和全髋(TH)的BMD相对于基线的变化以及椎体骨折风险。
结果
我们在该分析中识别并纳入了15项研究。除利塞膦酸盐外,所有BMA与未使用BMA的组相比,LS的BMD均显著增加,其中唑来膦酸盐的BMD增加最多。在TH,双膦酸盐类药物(阿仑膦酸盐、帕米膦酸盐和唑来膦酸盐)和地诺单抗与未使用BMA的组相比有显著升高。地诺单抗在TH处的BMD增加最多。只有地诺单抗降低了椎体骨折风险(相对风险[95%置信区间]:0.40[0.20 - 0.81])。尽管唑来膦酸盐在LS处的BMD增加最高,但在该分析中它并未降低椎体骨折风险。
结论
大多数双膦酸盐类药物和地诺单抗在没有骨转移的前列腺癌ADT患者中显著增加了LS和TH的BMD。特别是,唑来膦酸盐和地诺单抗分别是在LS和TH处BMD增加方面最有效的BMA。然而,地诺单抗而非唑来膦酸盐是唯一显示出显著降低椎体骨折风险的BMA。我们需要进一步研究来检查骨质量的变化以及对非椎体和髋部骨折风险的影响。
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