接受间歇性雄激素抑制治疗的前列腺癌患者骨转换的测量。

Open Access Journal of Urology Pub Date : 2010-09-07 eCollection Date: 2010-01-01 DOI:10.2147/OAJU.S13046
Gerhard Theyer, Stefan Holub, Ulrike Olszewski, Gerhard Hamilton
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引用次数: 3

摘要

目的:对接受间歇雄激素抑制治疗(IAS)的前列腺癌患者骨密度(BMD)的临床测量报告表明,与持续雄激素抑制治疗(CAS)相比,接受间歇雄激素抑制治疗(IAS)允许在治疗周期之间激素恢复,骨质疏松症减少。在本研究中,通过测定胶原降解的生化标志物CrossLaps,研究了IAS对骨代谢的影响。方法:对75例≥pT2期前列腺癌患者进行100个IAS治疗周期的研究。临床资料和每月实验室检查(睾酮、前列腺特异性抗原;使用CrossLaps®酶联免疫吸附试验(ELISA)检测这些患者的PSA和c端末端肽胶原片段。结果:在雄激素抑制(AS)阶段持续9个月的血清睾酮(结论:接受IAS的前列腺癌患者的血清CrossLaps浓度测量表明,治疗停止阶段迅速逆转了与AS阶段相关的骨退化增加,与临床观察报告相比,IAS减少了骨密度损失。就临床结果而言,IAS似乎与CAS一样有效,但副作用更少,正如雄激素诱导的骨基质降解减少所证明的那样。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Measurement of bone turnover in prostate cancer patients receiving intermittent androgen suppression therapy.

Measurement of bone turnover in prostate cancer patients receiving intermittent androgen suppression therapy.

Measurement of bone turnover in prostate cancer patients receiving intermittent androgen suppression therapy.

Purpose: Reports on clinical measurements of bone mineral density (BMD) in prostate cancer patients undergoing intermittent androgen suppression therapy (IAS) that allows for hormonal recovery between treatment cycles indicate decreased osteoporosis compared to continuous androgen suppression therapy (CAS). In the present study the effect of IAS on bone metabolism by determinations of CrossLaps, a biochemical marker of collagen degradation, were examined.

Method: In total 100 IAS treatment cycles of 75 patients with prostate cancer stages ≥ pT2 were studied. Clinical data and monthly laboratory tests (testosterone, prostate-specific antigen; PSA) of these patients were monitored together with measurements of C-terminal telopeptide collagen fragments using CrossLaps® ELISA assays.

Results: During phases of androgen suppression (AS) lasting for 9 months serum testosterone (<1 ng/mL) and PSA (<2 ng/mL) levels were reversibly reduced, indicating partial growth arrest and apoptotic regression of the prostatic tumors. Serum CrossLaps concentrations peaked at the last 2 months of the AS phases (0.91 ± 0.25 μg/L; mean ± SEM) and were reduced below initial values (0.21 ± 0.43 versus baseline of 0.43 ± 0.06 μg/L) during therapy cessation periods until tumor progression-related increases.

Conclusion: Measurements of the serum concentration of CrossLaps in prostate cancer patients receiving IAS indicated that treatment cessation phases rapidly reversed increased bone degradation associated with AS phases, in strong agreement with the clinical observations reporting reduced loss of BMD in IAS when compared to CAS. In terms of clinical outcomes, IAS seems to be as effective as CAS while showing reduced side effects, as demonstrated here by the reduction of androgen-induced bone matrix degradation.

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