Lipton Allan, Cook Richard, Saad Fred, Major Pierre, Garnero Patrick, Terpos Evangelos, Brown Janet E, Coleman Robert E
Department of Hematology-Oncology, Milton S. Hershey Medical Center, Pennsylvania State University, Hershey, PA 17033, USA.
Cancer. 2008 Jul 1;113(1):193-201. doi: 10.1002/cncr.23529.
For patients with bone metastases, high N-telopeptide of type I collagen (NTX) levels correlate with increased risks of skeletal-related events and death. However, the relation between NTX decreases and clinical benefits is unclear.
Correlations between NTX normalization during treatment and clinical outcome were retrospectively analyzed in 3 large, phase 3 trials. Urinary NTX levels were measured at baseline and at Month 3 in patients with bone metastases from breast cancer (BC; n = 578), hormone-refractory prostate cancer (HRPC; n = 472), or nonsmall-cell lung cancer and other solid tumors (NSCLC/OST; n = 291) who received zoledronic acid or control (pamidronate for BC; placebo for HRPC and NSCLC/OST) for up to 24 months. NTX levels were characterized as normal (N; <64 nmol/mmol creatinine) or elevated (E; > or =64 nmol/mmol creatinine).
After 3 months of zoledronic acid, most N-group patients maintained normal levels; however, most E-group patients normalized their NTX levels (BC, 81%; HRPC, 70%; NSCLC/OST, 81%). In contrast, NTX levels normalized with pamidronate in 65% of BC, with placebo in 8% of HRPC, and in 17% of NSCLC/OST E-group patients. Normalized NTX correlated with improved overall survival versus persistently elevated NTX (significant for zoledronic acid-treated patients; trend for placebo-treated patients). Moreover, percentage reductions from baseline NTX levels correlated with benefits regardless of whether patients transitioned from E to N.
Zoledronic acid normalizes or maintains normal NTX levels in most patients with bone metastases. Normalized NTX within 3 months of treatment, versus persistently elevated NTX, was associated with reduced risks of skeletal complications and death.
对于骨转移患者,I型胶原N-端肽(NTX)水平升高与骨相关事件及死亡风险增加相关。然而,NTX水平降低与临床获益之间的关系尚不清楚。
在3项大型3期试验中,对治疗期间NTX水平正常化与临床结局之间的相关性进行回顾性分析。对患有乳腺癌(BC;n = 578)、激素难治性前列腺癌(HRPC;n = 472)或非小细胞肺癌及其他实体瘤(NSCLC/OST;n = 291)的骨转移患者,在基线及治疗3个月时测量尿NTX水平,这些患者接受唑来膦酸或对照治疗(BC用帕米膦酸;HRPC和NSCLC/OST用安慰剂)长达24个月。NTX水平分为正常(N;<64 nmol/mmol肌酐)或升高(E;≥64 nmol/mmol肌酐)。
唑来膦酸治疗3个月后,大多数N组患者维持正常水平;然而,大多数E组患者的NTX水平恢复正常(BC为81%;HRPC为70%;NSCLC/OST为81%)。相比之下,BC患者中65%用帕米膦酸后NTX水平恢复正常,HRPC患者中8%用安慰剂后NTX水平恢复正常,NSCLC/OST E组患者中17%用安慰剂后NTX水平恢复正常。NTX水平恢复正常与总体生存率改善相关,与持续升高的NTX相比(唑来膦酸治疗患者有显著差异;安慰剂治疗患者有趋势差异)。此外,无论患者NTX水平是从E转变为N,基线NTX水平的降低百分比均与获益相关。
唑来膦酸可使大多数骨转移患者的NTX水平恢复正常或维持正常。治疗3个月内NTX水平恢复正常,与持续升高相比,与骨并发症及死亡风险降低相关。
