Antonarakis Emmanuel S, Heath Elisabeth I, Walczak Janet R, Nelson William G, Fedor Helen, De Marzo Angelo M, Zahurak Marianna L, Piantadosi Steven, Dannenberg Andrew J, Gurganus Robin T, Baker Sharyn D, Parnes Howard L, DeWeese Theodore L, Partin Alan W, Carducci Michael A
Sidney Kimmel Comprehensive Cancer Center, Johns Hopkins School of Medicine, Baltimore, MD 21231, USA.
J Clin Oncol. 2009 Oct 20;27(30):4986-93. doi: 10.1200/JCO.2009.21.9410. Epub 2009 Aug 31.
Cyclooxygenase-2 (COX-2) is a potential pharmacologic target for the prevention of various malignancies, including prostate cancer. We conducted a randomized, double-blind trial to examine the effect of celecoxib on drug-specific biomarkers from prostate tissue obtained at prostatectomy.
Patients with localized prostate cancer and Gleason sum > or = 7, prostate-specific antigen (PSA) > or = 15 ng/mL, clinical stage T2b or greater, or any combination with greater than 45% risk of capsular penetration were randomly assigned to celecoxib 400 mg by mouth twice daily or placebo for 4 to 6 weeks before prostatectomy. The primary end point was the difference in prostatic prostaglandin levels between the two groups. Secondary end points were differences in COX-1 and -2 expressions; oxidized DNA bases; and markers of proliferation, apoptosis and angiogenesis. Tissue celecoxib concentrations also were measured. Tertiary end points were drug safety and compliance.
Seventy-three patients consented, and 64 were randomly assigned and included in the intention-to-treat analysis. There were no treatment differences in any of the primary or secondary outcomes. Multivariable regression revealed that tumor tissue had significantly lower COX-2 expression than benign prostatic tissue (P = .01) and significantly higher levels of the proliferation marker Ki-67 (P < .0001). Celecoxib was measurable in prostate tissue of patients on treatment, demonstrating that celecoxib reached its target. Celecoxib was safe and resulted in only grade 1 toxicities.
Treatment with 4 to 6 weeks of celecoxib had no effect on intermediate biomarkers of prostate carcinogenesis, despite the achievement of measurable tissue levels. We caution against using celecoxib 400 mg twice daily as a preventive agent for prostate cancer in additional studies.
环氧化酶-2(COX-2)是预防包括前列腺癌在内的各种恶性肿瘤的潜在药理学靶点。我们进行了一项随机双盲试验,以研究塞来昔布对前列腺切除术中获取的前列腺组织中药物特异性生物标志物的影响。
局部前列腺癌且 Gleason 评分≥7、前列腺特异性抗原(PSA)≥15 ng/mL、临床分期为 T2b 或更高,或任何具有超过 45% 包膜穿透风险组合的患者,在前列腺切除术前随机分配至每日口服两次 400 mg 塞来昔布组或安慰剂组,持续 4 至 6 周。主要终点是两组之间前列腺前列腺素水平的差异。次要终点是 COX-1 和 -2 表达、氧化 DNA 碱基以及增殖、凋亡和血管生成标志物的差异。还测量了组织塞来昔布浓度。三级终点是药物安全性和依从性。
73 名患者同意参与,64 名被随机分配并纳入意向性分析。在任何主要或次要结局中均无治疗差异。多变量回归显示,肿瘤组织的 COX-2 表达明显低于良性前列腺组织(P = 0.01),增殖标志物 Ki-67 的水平明显更高(P < 0.0001)。治疗患者的前列腺组织中可检测到塞来昔布,表明塞来昔布达到了其靶点。塞来昔布是安全的,仅导致 1 级毒性。
尽管达到了可测量的组织水平,但 4 至 6 周的塞来昔布治疗对前列腺癌发生的中间生物标志物没有影响。我们提醒在其他研究中不要将每日两次 400 mg 塞来昔布用作前列腺癌的预防药物。