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Bendamustine with or without rituximab for the treatment of heavily pretreated non-Hodgkin's lymphoma patients : A multicenter retrospective study on behalf of the Italian Lymphoma Foundation (FIL).苯达莫司汀联合或不联合利妥昔单抗治疗经大量预处理的非霍奇金淋巴瘤患者:一项代表意大利淋巴瘤基金会(FIL)的多中心回顾性研究。
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利妥昔单抗、奥法木单抗及其他用于慢性淋巴细胞白血病的抗CD20单克隆抗体

Rituximab, ofatumumab and other monoclonal anti-CD20 antibodies for chronic lymphocytic leukaemia.

作者信息

Bauer Kathrin, Rancea Michaela, Roloff Verena, Elter Thomas, Hallek Michael, Engert Andreas, Skoetz Nicole

机构信息

Cochrane Haematological Malignancies Group, Department I of Internal Medicine, University Hospital of Cologne, Cologne,Germany.

出版信息

Cochrane Database Syst Rev. 2012 Nov 14;11(11):CD008079. doi: 10.1002/14651858.CD008079.pub2.

DOI:10.1002/14651858.CD008079.pub2
PMID:23152253
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6485963/
Abstract

BACKGROUND

Chronic lymphocytic leukaemia (CLL) accounts for 25% of all leukaemias and is the most common lymphoid malignancy in western countries. Standard treatments include mono- or polychemotherapies, usually combined with monoclonal antibodies such as rituximab or alemtuzumab. However, the impact of these agents remains unclear, as there are hints for increased risk of severe infections.

OBJECTIVES

The objectives of this review are to provide an evidence-based answer regarding the clinical benefits and harms of monoclonal anti-CD20 antibodies (such as rituximab, ofatumumab, GA101) compared to no further therapy or to other anti-leukaemic therapies in patients with CLL, irrespective of disease status.

SEARCH METHODS

We searched the Cochrane Central Register of Controlled Trials (The Cochrane Library Issue 12, 2011), MEDLINE (from January 1990 to 4 January 2012), and EMBASE (from 1990 to 20 March 2009) as well as conference proceedings (American Society of Hematology, American Society of Clinical Oncology, European Hematology Association and European Society of Medical Oncology) for randomised controlled trials (RCTs).

SELECTION CRITERIA

We included RCTs examining monoclonal anti-CD20 antibodies compared to no further therapy or to anti-leukaemic therapy such as chemotherapy or monoclonal antibodies in patients with newly diagnosed or relapsed CLL.

DATA COLLECTION AND ANALYSIS

We used hazard ratios (HR) as effect measures for overall survival (OS), progression-free survival (PFS) and time to next treatment, and risk ratios (RR) for response rates, treatment-related mortality (TRM) and adverse events (AEs). Two review authors independently extracted data and assessed quality of trials.

MAIN RESULTS

We screened a total of 1150 records. Seven RCTs involving 1763 patients were identified, but only five could be included in the two separate meta-analyses we performed. We judged the overall the quality of these trials as moderate to high. All trials were randomised and open-label studies. However, two trials were published as abstracts only, therefore we were unable to assess the potential risk of bias for these trials in detail.Three RCTs (N = 1421) assessed the efficacy of monoclonal anti-CD20 antibodies (i.e. rituximab) plus chemotherapy compared to chemotherapy alone. The meta-analyses showed a statistically significant OS (HR 0.78, 95% confidence interval (CI) 0.62 to 0.98, P = 0.03, the number needed to treat for an additional beneficial effect (NNTB) was 12) and PFS (HR 0.64, 95% CI 0.55 to 0.74, P < 0.00001) advantage for patients receiving rituximab. In the rituximab-arm occurred more AEs, World Health Organization (WHO) grade 3 or 4 (3 trials, N = 1398, RR 1.15, 95% CI 1.08 to 1.23, P < 0.0001; the number needed to harm for an additional harmful outcome (NNTH) was 9), but that did not lead to a statistically significant difference regarding TRM (3 trials, N = 1415, RR 1.19, 95% CI 0.70 to 2.01, P = 0.52).Two trials (N = 177) evaluated rituximab versus alemtuzumab. Neither study reported OS or PFS. There was no statistically significant difference between arms regarding complete response rate (CRR) (RR 1.21, 95% CI 0.94 to 1.58, P = 0.14) or TRM (RR 0.31, 95% CI 0.06 to 1.51, P = 0.15). However, the CLL2007FMP trial was stopped early owing to an increase in mortality in the alemtuzumab arm. More serious AEs occurred in this arm (43% with alemtuzumab versus 22% with rituximab; P = 0.006).Two trials assessed different dosages or time schedules of monoclonal anti-CD20 antibodies. One trial (N = 104) evaluated two different rituximab schedules (concurrent arm: fludarabine plus rituximab (Flu-R) plus rituximab consolidation versus sequential arm: fludarabine alone plus rituximab consolidation). The comparison of the concurrent versus sequential regimen of rituximab showed a statistically significant difference of the CRR with 33% in the concurrent-arm and 15% in the sequential-arm (P = 0.04), that did not lead to statistically significant differences regarding OS (HR 1.14, 95% CI 0.20 to 6.65, P = 0.30) or PFS (HR 0.96, 95% CI 0.43 to 2.15, P = 0.11). Furthermore results showed no differences in occurring AEs, except for neutropenia, which was more often observed in patients of the concurrent arm. The other trial (N = 61) investigated two different dosages (500 mg and 1000 mg) of ofatumumab in addition to FluC. The arm investigating ofatumumab did not assess OS and a median PFS had not been reached owing to the short median follow-up of eight months. It showed no statistically significant differences between arms regarding CRR (32% in the FCO500 arm versus 50% in the FCO1000 arm; P = 0.10) or AEs (anaemia, neutropenia, thrombocytopenia).

AUTHORS' CONCLUSIONS: This meta-analysis showed that patients receiving chemotherapy plus rituximab benefit in terms of OS as well as PFS compared to those with chemotherapy alone. Therefore, it supports the recommendation of rituximab in combination with FluC as an option for the first-line treatment as well as for the people with relapsed or refractory CLL. The available evidence regarding the other assessed comparisons was not sufficient to deduct final conclusions.

摘要

背景

慢性淋巴细胞白血病(CLL)占所有白血病的25%,是西方国家最常见的淋巴系统恶性肿瘤。标准治疗包括单药或多药化疗,通常联合使用利妥昔单抗或阿仑单抗等单克隆抗体。然而,这些药物的影响仍不明确,因为有迹象表明严重感染风险增加。

目的

本综述的目的是提供基于证据的答案,比较单克隆抗CD20抗体(如利妥昔单抗、奥法木单抗、GA101)与不进行进一步治疗或其他抗白血病治疗相比,对CLL患者的临床益处和危害,无论疾病状态如何。

检索方法

我们检索了Cochrane对照试验中心注册库(2011年第12期Cochrane图书馆)、MEDLINE(1990年1月至2012年1月4日)、EMBASE(1990年至2009年3月20日)以及会议论文集(美国血液学会、美国临床肿瘤学会、欧洲血液学协会和欧洲医学肿瘤学会),以查找随机对照试验(RCT)。

入选标准

我们纳入了比较单克隆抗CD20抗体与不进行进一步治疗或与抗白血病治疗(如化疗或单克隆抗体)相比的RCT,研究对象为新诊断或复发的CLL患者。

数据收集与分析

我们使用风险比(HR)作为总生存期(OS)、无进展生存期(PFS)和下次治疗时间的效应量,使用风险率(RR)作为缓解率、治疗相关死亡率(TRM)和不良事件(AE)的效应量。两位综述作者独立提取数据并评估试验质量。

主要结果

我们共筛选了1150条记录。确定了7项涉及1763例患者的RCT,但只有5项可纳入我们进行的两项单独的荟萃分析。我们认为这些试验的总体质量为中等到高。所有试验均为随机开放标签研究。然而,两项试验仅以摘要形式发表,因此我们无法详细评估这些试验的潜在偏倚风险。三项RCT(N = 1421)评估了单克隆抗CD20抗体(即利妥昔单抗)联合化疗与单纯化疗相比的疗效。荟萃分析显示,接受利妥昔单抗治疗的患者在OS(HR 0.78,95%置信区间(CI)0.62至0.98,P = 0.03,额外有益效果所需治疗人数(NNTB)为12)和PFS(HR 0.64,95%CI 0.55至0.74,P < 0.00001)方面具有统计学显著优势。在利妥昔单抗组发生的AE更多,世界卫生组织(WHO)3级或4级(3项试验,N = 1398,RR 1.15,95%CI 1.08至1.23,P < 0.0001;额外有害结果所需伤害人数(NNTH)为9),但这并未导致TRM方面的统计学显著差异(3项试验,N = 1415,RR 1.19,95%CI 0.70至2.01,P = 0.52)。两项试验(N = 177)评估了利妥昔单抗与阿仑单抗。两项研究均未报告OS或PFS。两组在完全缓解率(CRR)(RR 1.21,95%CI 0.94至1.58,P = 0.14)或TRM(RR 0.31,95%CI 0.06至1.51,P = 0.15)方面无统计学显著差异。然而,CLL2007FMP试验因阿仑单抗组死亡率增加而提前终止。该组发生的更严重AE更多(阿仑单抗组为43%,利妥昔单抗组为22%;P = 0.006)。两项试验评估了单克隆抗CD20抗体的不同剂量或时间方案。一项试验(N = 104)评估了两种不同的利妥昔单抗方案(同步组:氟达拉滨加利妥昔单抗(Flu-R)加利妥昔单抗巩固治疗与序贯组:单独氟达拉滨加利妥昔单抗巩固治疗)。利妥昔单抗同步与序贯方案的比较显示,CRR有统计学显著差异,同步组为33%,序贯组为15%(P = 0.04),但这并未导致OS(HR 1.14,95%CI 0.20至6.65,P = 0.30)或PFS(HR 0.96,95%CI 0.43至2.15,P = 0.11)方面的统计学显著差异。此外,结果显示除中性粒细胞减少外,AE发生情况无差异,中性粒细胞减少在同步组患者中更常观察到。另一项试验(N = 61)除FluC外,研究了奥法木单抗的两种不同剂量(500 mg和1000 mg)。研究奥法木单抗的组未评估OS,由于中位随访时间仅8个月,未达到中位PFS。两组在CRR(FCO500组为32%,FCO1000组为50%;P = 0.10)或AE(贫血、中性粒细胞减少、血小板减少)方面无统计学显著差异。

作者结论

本荟萃分析表明,与单纯化疗相比,接受化疗加利妥昔单抗治疗的患者在OS和PFS方面均有益处。因此,它支持推荐利妥昔单抗联合FluC作为一线治疗以及复发或难治性CLL患者的一种选择。关于其他评估比较的现有证据不足以得出最终结论。