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[前列腺癌转移性骨病及治疗所致骨质疏松的治疗。骨保护策略的演变]

[Treatment of metastatic bone disease and treatment-induced osteoporosis in prostate cancer. Evolution of osteoprotective strategies].

作者信息

Todenhöfer T, Schwentner C, Schilling D, Gakis G, Stenzl A

机构信息

Klinik für Urologie, Universitätsklinikum Tübingen, Hoppe-Seyler-Straße 1, 72076, Tübingen, Deutschland.

出版信息

Urologe A. 2011 Sep;50(9):1055-63. doi: 10.1007/s00120-011-2623-6.

Abstract

Patients with prostate cancer and bone metastases on average experience one skeletal-related event per year. To avoid complications caused by bone metastases and androgen deprivation therapy-induced osteoporosis, which lead to significant increases in costs and mortality, bone metabolism can be influenced in several ways. Bisphosphonates, which directly inhibit signalling pathways in osteoclasts, can reduce the rate of skeletal-related events in metastatic prostate cancer. The RANKL antibody denosumab inhibits the crosstalk between osteoblasts, osteoclasts and tumour cells and has been shown to reduce the rate of vertebral fractures in patients with treatment-induced osteoporosis. Furthermore, it has been recently shown to prevent skeletal-related events in prostate cancer patients with metastatic bone disease. In patients with castration resistant prostate cancer, denosumab prolongs bone-metastasis-free-survival. Whereas ample data are available about side effects of bisphosphonates, limited evidence exists about the long-term safety profile of denosumab. Therefore, a thorough patient selection is advocated for therapeutic application of denosumab in patients with prostate cancer.

摘要

患有前列腺癌和骨转移的患者平均每年经历一次骨相关事件。为避免骨转移和雄激素剥夺治疗引起的骨质疏松症所导致的并发症,这些并发症会使成本和死亡率显著增加,可以通过多种方式影响骨代谢。双膦酸盐直接抑制破骨细胞中的信号通路,可降低转移性前列腺癌骨相关事件的发生率。RANKL抗体地诺单抗可抑制成骨细胞、破骨细胞和肿瘤细胞之间的相互作用,已证明可降低治疗性骨质疏松症患者的椎体骨折发生率。此外,最近还证明它可预防患有转移性骨病的前列腺癌患者发生骨相关事件。在去势抵抗性前列腺癌患者中,地诺单抗可延长无骨转移生存期。虽然有大量关于双膦酸盐副作用的数据,但关于地诺单抗长期安全性的证据有限。因此,主张对前列腺癌患者进行地诺单抗治疗应用的全面患者选择。

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