Wuntakal Rekha, Seshadri Srividya, Montes Ana, Lane Geoff
Gynaecological Oncology, Barking, Havering & Redbridge University Hospitals NHS Trust, Rom Valley Way, Romford, UK, RM7 0AG.
Cochrane Database Syst Rev. 2016 Jun 29;2016(6):CD011322. doi: 10.1002/14651858.CD011322.pub2.
Ovarian cancer is seventh most common cancer in women worldwide. Approximately 1.3% of women will be diagnosed with ovarian cancer at some point during their life time. The majority of tumours arise from surface of the ovary (epithelial). Two thirds of these women will present with advanced disease, requiring aggressive treatment, which includes debulking surgery (removal of as much disease as possible) and chemotherapy. However, most women (75%) with advanced epithelial ovarian cancer (EOC) will relapse following surgery and chemotherapy. Patients who relapse are treated with either platinum or non-platinum drugs and this is dependent on the platinum-sensitivity and platinum-free interval. These drug regimens are generally well-tolerated although there are potential severe side effects. New treatments that can be used to treat recurrence or prevent disease progression after first-line or subsequent chemotherapy are important, especially those with a low toxicity profile. Hormones such as luteinising hormone releasing hormone (LHRH) agonists have been used in the treatment of relapsed EOC. Some studies have shown objective remissions, while other studies have shown little or no benefit. Most small studies report a better side-effect profile for LHRH agonists when compared to standard chemotherapeutic agents used in EOC.
To compare the effectiveness and safety of luteinising hormone releasing hormone (LHRH) agonists with chemotherapeutic agents or placebo in relapsed epithelial ovarian cancer (EOC).
We searched the Cochrane Gynaecological Cancer Group trials register, Cochrane Central Register of Controlled Trials (CENTRAL), MEDLINE and Embase up to January 2016. We also searched registers of clinical trials and abstracts of scientific meetings.
Randomised controlled trials (RCTs) that compared LHRH agonists with chemotherapeutic agents or placebo in relapsed EOC.
Two review authors independently assessed whether relevant studies met the inclusion criteria, retrieved data and assessed risk of bias.
Two studies, including 97 women, met our inclusion criteria: one assessed LHRH agonist (leuprorelin) use in relapsed (platinum-resistant and platinum-refractory) EOC in comparison with a chemotherapeutic agent (treosulfan) (Du Bois 2002); the other examined LHRH agonist (decapeptyl) versus a placebo (Currie 1994). Since both studies had different control groups, a meta-analysis was not possible.There may be little or no difference between treatment with leuprorelin or treosulfan in overall survival (OS) (hazard ratio (HR) 0.98, 95% confidence interval (CI) 0.58 to 1.67; very low-quality evidence) or progression-free survival (PFS) at six and 12 months (risk ratio (RR) 0.61, 95% CI 0.22 to 1.68, and RR 0.65, 95% CI 0.12 to 3.66; very low-quality evidence), respectively (Du Bois 2002). The duration of follow-up was 2.5 years and quality of life (QoL) was not reported in this study.Alopecia and fatigue were probably more common with treosulfan than leuprorelin (alopecia RR 0.32, 95% CI 0.12 to 0.91 (very low-quality evidence)). There may be little or no difference in other Grade 3/4 side effects: nausea and vomiting (RR 0.65, 95% CI 0.12 to 3.66 (very low-quality evidence)); neurotoxicity (RR 0.32, 95% CI 0.01 to 7.71 (very low-quality evidence)) and neutropenia (RR 0.97, 95% 0.06 to 14.97 (very low-quality evidence)),The Currie 1994 study, which compared decapeptyl treatment with placebo, reported mean PFS of 16 weeks verus 11.2 weeks, respectively. No relative effects measures or P value at a particular time point were reported. Overall survival (OS) and QoL outcomes were not reported. In addition, adverse events were only mentioned for the decapeptyl group.Adverse events were incompletely reported (no adverse events in decapeptyl group, but not reported for the placebo group).
AUTHORS' CONCLUSIONS: Based on this review of two small RCTs, there is not enough evidence to comment on the safety and effectiveness of LHRH agonists in the treatment of platinum-refractory and platinum-resistant (relapsed) EOC. Overall, the quality of evidence for all outcomes (including OS, PFS, QoL and adverse events) is very low.
卵巢癌是全球女性中第七大常见癌症。约1.3%的女性在其一生中的某个阶段会被诊断为卵巢癌。大多数肿瘤起源于卵巢表面(上皮性)。这些女性中有三分之二会出现晚期疾病,需要积极治疗,包括肿瘤细胞减灭术(尽可能切除更多病灶)和化疗。然而,大多数晚期上皮性卵巢癌(EOC)女性(75%)在手术和化疗后会复发。复发患者接受铂类或非铂类药物治疗,这取决于铂敏感性和无铂间期。这些药物方案一般耐受性良好,尽管存在潜在的严重副作用。可用于治疗复发或预防一线或后续化疗后疾病进展的新疗法很重要,尤其是那些毒性较低的疗法。促黄体生成素释放激素(LHRH)激动剂等激素已用于复发性EOC的治疗。一些研究显示有客观缓解,而其他研究显示获益甚微或无获益。与用于EOC的标准化疗药物相比,大多数小型研究报告LHRH激动剂的副作用较小。
比较促黄体生成素释放激素(LHRH)激动剂与化疗药物或安慰剂在复发性上皮性卵巢癌(EOC)中的有效性和安全性。
我们检索了Cochrane妇科癌症组试验注册库、Cochrane对照试验中央注册库(CENTRAL)、MEDLINE和Embase,检索截止至2016年1月。我们还检索了临床试验注册库和科学会议摘要。
比较LHRH激动剂与化疗药物或安慰剂在复发性EOC中的随机对照试验(RCT)。
两位综述作者独立评估相关研究是否符合纳入标准,检索数据并评估偏倚风险。
两项研究(共97名女性)符合我们的纳入标准:一项研究评估了LHRH激动剂(亮丙瑞林)在复发性(铂耐药和铂难治性)EOC中的应用,并与化疗药物(苏消安)进行比较(Du Bois 2002);另一项研究比较了LHRH激动剂(醋酸曲普瑞林)与安慰剂(Currie 1994)。由于两项研究的对照组不同,无法进行荟萃分析。在总生存期(OS)方面,亮丙瑞林或苏消安治疗之间可能几乎没有差异(风险比(HR)0.98,95%置信区间(CI)0.58至1.67;极低质量证据),在6个月和12个月的无进展生存期(PFS)方面也可能几乎没有差异(风险比(RR)0.61,95%CI 0.22至1.68,以及RR 0.65,95%CI 0.12至3.66;极低质量证据)(Du Bois 2002)。随访时间为2.5年,本研究未报告生活质量(QoL)。脱发和疲劳可能在使用苏消安的患者中比使用亮丙瑞林的患者更常见(脱发RR 0.32,95%CI 0.12至0.91(极低质量证据))。在其他3/4级副作用方面可能几乎没有差异:恶心和呕吐(RR 0.65,95%CI 0.12至3.66(极低质量证据));神经毒性(RR 0.32,95%CI 0.01至7.71(极低质量证据))和中性粒细胞减少(RR 0.97,95%CI 0.06至14.97(极低质量证据))。Currie 1994年的研究比较了醋酸曲普瑞林治疗与安慰剂,分别报告平均PFS为16周和11.2周。未报告特定时间点的相对效应量或P值。未报告总生存期(OS)和生活质量(QoL)结果。此外,仅提及了醋酸曲普瑞林组的不良事件。不良事件报告不完整(醋酸曲普瑞林组无不良事件,但安慰剂组未报告)。
基于对两项小型RCT的综述,没有足够的证据来评价LHRH激动剂在治疗铂难治性和铂耐药性(复发性)EOC中的安全性和有效性。总体而言,所有结局(包括OS、PFS、QoL和不良事件)的证据质量都非常低。
