铂耐药卵巢癌患者疾病进展时 CA-125 与 RECIST 之间的一致性差:AURELIA 试验分析。
Poor concordance between CA-125 and RECIST at the time of disease progression in patients with platinum-resistant ovarian cancer: analysis of the AURELIA trial.
机构信息
NSGO and Department of Gynecological Cancer, The Norwegian Radium Hospital, Oslo University Hospital, Oslo
NSGO and Department of Gynecological Cancer and Institute for Cancer Genetics and Informatics, The Norwegian Radium Hospital, Oslo University Hospital and Institute for Clinical Medicine, Oslo University, Oslo, Norway.
出版信息
Ann Oncol. 2016 Aug;27(8):1505-10. doi: 10.1093/annonc/mdw238. Epub 2016 Jul 11.
BACKGROUND
Data on CA-125 as a predictor of disease progression (PD) in ovarian cancer come predominantly from patients with platinum-sensitive disease receiving chemotherapy alone. We assessed concordance between CA-125-defined and RECIST-defined PD using data from the Gynecologic Cancer InterGroup (GCIG) randomized phase III AURELIA trial in platinum-resistant ovarian cancer (PROC).
PATIENTS AND METHODS
Patients with PROC were randomized to receive single-agent chemotherapy with or without bevacizumab. PD by CA-125 was defined according to GCIG criteria (except that confirmatory CA-125 measurement was not required). This exploratory analysis included patients with RECIST PD and a CA-125 reading ≤28 days before and ≤21 days after RECIST-defined PD.
RESULTS
Of 218 eligible patients, only 94 (43%, 95% confidence interval 36% to 50%) had concordant RECIST and CA-125 PD status (42% in the chemotherapy-alone arm; 45% in the bevacizumab combination arm, P = 0.6). There was no evidence of CA-125-defined PD in the remaining 124 patients despite PD according to imaging. There were no significant differences in baseline characteristics between patients with PD defined by both RECIST and CA-125 and those with RECIST-only PD. CA-125 was even less sensitive in detecting PD in patients with early (<8 weeks after randomization) compared with later RECIST-defined PD (69% versus 53%, respectively, not meeting CA-125 criteria; P = 0.053). There was no significant difference in survival after PD in patients with concordant PD by RECIST and CA-125 versus those with PD only by RECIST. We validated our findings in an independent study population of PROC.
CONCLUSIONS
In this platinum-resistant population, PD was typically detected earlier by imaging than by CA-125, irrespective of bevacizumab treatment. Disease status by CA-125 at the time of PD was not prognostic for overall survival. Regular radiologic assessment as well as symptom benefit assessment should be considered during PROC follow-up.
背景
CA-125 作为预测卵巢癌疾病进展(PD)的标志物,主要来源于接受单纯化疗的铂敏感疾病患者。我们使用来自卵巢癌妇科癌症团体(GCIG)随机 III 期 AURELIA 试验铂耐药卵巢癌(PROC)的数据,评估 CA-125 定义的 PD 与 RECIST 定义的 PD 的一致性。
患者和方法
PROC 患者随机接受单药化疗加或不加贝伐单抗。CA-125 定义的 PD 根据 GCIG 标准(除了不需要确认 CA-125 测量)。这项探索性分析包括 RECIST PD 患者和 RECIST 定义的 PD 前≤28 天和后≤21 天 CA-125 读数≤28 天的患者。
结果
在 218 名合格患者中,只有 94 名(43%,95%置信区间 36%至 50%)具有 RECIST 和 CA-125 PD 状态的一致性(化疗组为 42%;贝伐单抗联合组为 45%,P=0.6)。在其余 124 名患者中,尽管根据影像学检查结果显示 PD,但没有证据表明存在 CA-125 定义的 PD。PD 同时根据 RECIST 和 CA-125 定义和仅根据 RECIST 定义的患者之间的基线特征没有显著差异。与 RECIST 定义的较晚 PD 相比,早期(随机分组后<8 周) CA-125 检测 PD 的敏感性更低(分别为 69%和 53%,未达到 CA-125 标准;P=0.053)。在 RECIST 和 CA-125 定义的 PD 一致的患者与仅 RECIST 定义的 PD 患者中,PD 后的生存没有显著差异。我们在 PROC 的另一个独立研究人群中验证了我们的发现。
结论
在这个铂耐药人群中,无论是否接受贝伐单抗治疗,PD 通常都比 CA-125 更早被影像学检测到。PD 时 CA-125 的疾病状态与总生存期无关。在 PROC 随访期间,应考虑常规影像学评估和症状获益评估。
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