University of Illinois at Chicago, Chicago, IL, USA.
Curr Med Res Opin. 2011 Jan;27(1):55-62. doi: 10.1185/03007995.2010.535511. Epub 2010 Nov 18.
To evaluate the effects of timing and length of zoledronic acid (ZA) treatment on outcomes for patients with prostate cancer in clinical practice.
Patients with prostate cancer and first bone metastasis diagnosed from January 2003 to October 2006 were included. Patients were considered 'untreated' if no ZA was given, 'early ZA-treated' if ZA was initiated before skeletal complication (SC) occurrence or 'late ZA-treated' if one or more SC was documented before or at ZA initiation. Patients were classified with short (≤ 90 days), medium (91-180 days) or long (>180 days) treatment persistence. Assessments included follow-up duration (FUP) and risk of developing one or more SC.
Among eligible patients, 847 were untreated, 243 were early ZA-treated and 218 were late ZA-treated. For untreated versus early ZA-treated groups, median FUP was 263 versus 357 days (p < 0.0001), respectively, and time to first SC was 199 versus 273 days (p < 0.0001), respectively. ZA treatment was associated with significantly longer FUP and lower SC risk. The early ZA-treated group had significantly longer FUP versus the late ZA-treated group (median days, 357 vs. 299.5); the late ZA-treated group experienced significantly higher SC risk vs. the early ZA-treated group (odds ratio, 1.51). Compared with the long-persistence group, FUP was 56% and 40% shorter in the short and medium groups, respectively (p < 0.0001).
Treatment with and early initiation of ZA for patients with prostate cancer and bone metastasis significantly prolonged time to and reduced risk of developing SC, while extending FUP.
评估唑来膦酸(ZA)治疗的时机和时间长短对临床实践中前列腺癌患者结局的影响。
纳入 2003 年 1 月至 2006 年 10 月诊断为前列腺癌和首次骨转移的患者。如果未给予 ZA,则认为患者为“未治疗”;如果在发生骨骼并发症(SC)之前开始 ZA,则认为患者为“早期 ZA 治疗”;如果在开始 ZA 之前或同时发生了一个或多个 SC,则认为患者为“晚期 ZA 治疗”。将患者分为短期(≤90 天)、中期(91-180 天)或长期(>180 天)治疗持续时间。评估包括随访时间(FUP)和发生一个或多个 SC 的风险。
在符合条件的患者中,847 例为未治疗,243 例为早期 ZA 治疗,218 例为晚期 ZA 治疗。与未治疗组相比,早期 ZA 治疗组的中位 FUP 分别为 263 天和 357 天(p<0.0001),首次 SC 时间分别为 199 天和 273 天(p<0.0001)。ZA 治疗与更长的 FUP 和更低的 SC 风险相关。与晚期 ZA 治疗组相比,早期 ZA 治疗组的 FUP 显著延长(中位天数,357 天 vs. 299.5 天);晚期 ZA 治疗组的 SC 风险显著升高(优势比,1.51)。与长期持续组相比,短期和中期持续组的 FUP 分别缩短了 56%和 40%(p<0.0001)。
对于患有前列腺癌和骨转移的患者,ZA 的治疗和早期开始显著延长了发生 SC 的时间并降低了发生 SC 的风险,同时延长了 FUP。
