Valipour Arash, Jäger Manuel, Wu Peggy, Schmitt Jochen, Bunch Charles, Weberschock Tobias
Department of Dermatology, Venereology and Allergology, Johann Wolfgang Goethe-University Hospital, Frankfurt am Main, Germany.
Evidence-Based Medicine Frankfurt, Institute of General Practice, Goethe University, Frankfurt, Germany.
Cochrane Database Syst Rev. 2020 Jul 7;7(7):CD008946. doi: 10.1002/14651858.CD008946.pub3.
Mycosis fungoides (MF) is the most common type of cutaneous T-cell lymphoma, a malignant, chronic disease initially affecting the skin. Several therapies are available, which may induce clinical remission for a time. This is an update of a Cochrane Review first published in 2012: we wanted to assess new trials, some of which investigated new interventions.
To assess the effects of interventions for MF in all stages of the disease.
We updated our searches of the following databases to May 2019: the Cochrane Skin Specialised Register, CENTRAL, MEDLINE, Embase, and LILACS. We searched 2 trials registries for additional references. For adverse event outcomes, we undertook separate searches in MEDLINE in April, July and November 2017.
Randomised controlled trials (RCTs) of local or systemic interventions for MF in adults with any stage of the disease compared with either another local or systemic intervention or with placebo.
We used standard methodological procedures expected by Cochrane. The primary outcomes were improvement in health-related quality of life as defined by participants, and common adverse effects of the treatments. Key secondary outcomes were complete response (CR), defined as complete disappearance of all clinical evidence of disease, and objective response rate (ORR), defined as proportion of patients with a partial or complete response. We used GRADE to assess the certainty of evidence and considered comparisons of psoralen plus ultraviolet A (PUVA) light treatment as most important because this is first-line treatment for MF in most guidelines.
This review includes 20 RCTs (1369 participants) covering a wide range of interventions. The following were assessed as either treatments or comparators: imiquimod, peldesine, hypericin, mechlorethamine, nitrogen mustard and intralesional injections of interferon-α (IFN-α) (topical applications); PUVA, extracorporeal photopheresis (ECP: photochemotherapy), and visible light (light applications); acitretin, bexarotene, lenalidomide, methotrexate and vorinostat (oral agents); brentuximab vedotin; denileukin diftitox; mogamulizumab; chemotherapy with cyclophosphamide, doxorubicin, etoposide, and vincristine; a combination of chemotherapy with electron beam radiation; subcutaneous injection of IFN-α; and intramuscular injections of active transfer factor (parenteral systemics). Thirteen trials used an active comparator, five were placebo-controlled, and two compared an active operator to observation only. In 14 trials, participants had MF in clinical stages IA to IIB. All participants were treated in secondary and tertiary care settings, mainly in Europe, North America or Australia. Trials recruited both men and women, with more male participants overall. Trial duration varied from four weeks to 12 months, with one longer-term study lasting more than six years. We judged 16 trials as at high risk of bias in at least one domain, most commonly performance bias (blinding of participants and investigators), attrition bias and reporting bias. None of our key comparisons measured quality of life, and the two studies that did presented no usable data. Eighteen studies reported common adverse effects of the treatments. Adverse effects ranged from mild symptoms to lethal complications depending upon the treatment type. More aggressive treatments like systemic chemotherapy generally resulted in more severe adverse effects. In the included studies, CR rates ranged from 0% to 83% (median 31%), and ORR ranged from 0% to 88% (median 47%). Five trials assessed PUVA treatment, alone or combined, summarised below. There may be little to no difference between intralesional IFN-α and PUVA compared with PUVA alone for 24 to 52 weeks in CR (risk ratio (RR) 1.07, 95% confidence interval (CI) 0.87 to 1.31; 2 trials; 122 participants; low-certainty evidence). Common adverse events and ORR were not measured. One small cross-over trial found once-monthly ECP for six months may be less effective than twice-weekly PUVA for three months, reporting CR in two of eight participants and ORR in six of eight participants after PUVA, compared with no CR or ORR after ECP (very low-certainty evidence). Some participants reported mild nausea after PUVA but no numerical data were given. One participant in the ECP group withdrew due to hypotension. However, we are unsure of the results due to very low-certainty evidence. One trial comparing bexarotene plus PUVA versus PUVA alone for up to 16 weeks reported one case of photosensitivity in the bexarotene plus PUVA group compared to none in the PUVA-alone group (87 participants; low-certainty evidence). There may be little to no difference between bexarotene plus PUVA and PUVA alone in CR (RR 1.41, 95% CI 0.71 to 2.80) and ORR (RR 0.94, 95% CI 0.61 to 1.44) (93 participants; low-certainty evidence). One trial comparing subcutaneous IFN-α injections combined with either acitretin or PUVA for up to 48 weeks or until CR indicated there may be little to no difference in the common IFN-α adverse effect of flu-like symptoms (RR 1.32, 95% CI 0.92 to 1.88; 82 participants). There may be lower CR with IFN-α and acitretin compared with IFN-α and PUVA (RR 0.54, 95% CI 0.35 to 0.84; 82 participants) (both outcomes: low-certainty evidence). This trial did not measure ORR. One trial comparing PUVA maintenance treatment to no maintenance treatment, in participants who had already had CR, did report common adverse effects. However, the distribution was not evaluable. CR and OR were not assessable. The range of treatment options meant that rare adverse effects consequently occurred in a variety of organs.
AUTHORS' CONCLUSIONS: There is a lack of high-certainty evidence to support decision making in the treatment of MF. Because of substantial heterogeneity in design, missing data, small sample sizes, and low methodological quality, the comparative safety and efficacy of these interventions cannot be reliably established on the basis of the included RCTs. PUVA is commonly recommended as first-line treatment for MF, and we did not find evidence to challenge this recommendation. There was an absence of evidence to support the use of intralesional IFN-α or bexarotene in people receiving PUVA and an absence of evidence to support the use of acitretin or ECP for treating MF. Future trials should compare the safety and efficacy of treatments to PUVA, as the current standard of care, and should measure quality of life and common adverse effects.
蕈样肉芽肿(MF)是最常见的皮肤T细胞淋巴瘤类型,是一种最初累及皮肤的恶性慢性疾病。有多种治疗方法可供选择,这些方法可能会在一段时间内诱导临床缓解。这是对2012年首次发表的Cochrane系统评价的更新:我们希望评估新的试验,其中一些试验研究了新的干预措施。
评估疾病各阶段MF干预措施的效果。
我们更新了对以下数据库截至2019年5月的检索:Cochrane皮肤专科注册库、Cochrane系统评价数据库、医学期刊数据库、荷兰医学文摘数据库和拉丁美洲及加勒比地区卫生科学数据库。我们检索了2个试验注册库以获取更多参考文献。对于不良事件结局,我们于2017年4月、7月和11月在医学期刊数据库中进行了单独检索。
针对任何疾病阶段的成年MF患者的局部或全身干预的随机对照试验(RCT),与另一种局部或全身干预措施或安慰剂进行比较。
我们采用了Cochrane期望的标准方法程序。主要结局是参与者定义的健康相关生活质量改善情况以及治疗的常见不良反应。关键次要结局是完全缓解(CR),定义为疾病所有临床证据完全消失,以及客观缓解率(ORR),定义为部分或完全缓解患者的比例。我们使用GRADE评估证据的确定性,并认为补骨脂素加紫外线A(PUVA)光疗的比较最为重要,因为这是大多数指南中MF的一线治疗方法。
本综述纳入了20项RCT(1369名参与者),涵盖了广泛的干预措施。以下被评估为治疗或对照:咪喹莫特、培地西平、金丝桃素、氮芥、氮芥和病灶内注射干扰素-α(IFN-α)(局部应用);PUVA、体外光化学疗法(ECP:光化学疗法)和可见光(光应用);阿维A、贝沙罗汀、来那度胺、甲氨蝶呤和伏立诺他(口服制剂);本妥昔单抗;地尼白介素;莫加莫单抗;环磷酰胺、多柔比星、依托泊苷和长春新碱化疗;化疗与电子束放疗联合;皮下注射IFN-α;以及肌肉注射活性转移因子(胃肠外全身治疗)。13项试验使用了活性对照,5项为安慰剂对照,2项将活性治疗与仅观察进行了比较。在14项试验中,参与者处于临床IA至IIB期MF。所有参与者均在二级和三级医疗机构接受治疗,主要在欧洲、北美或澳大利亚。试验招募了男性和女性,总体上男性参与者更多。试验持续时间从4周至12个月不等,有一项长期研究持续超过6年。我们判断16项试验在至少一个领域存在高偏倚风险,最常见的是实施偏倚(参与者和研究者的盲法)、失访偏倚和报告偏倚。我们的关键比较均未测量生活质量,进行了此项测量的两项研究未提供可用数据。18项研究报告了治疗的常见不良反应。不良反应范围从轻微症状到致命并发症,取决于治疗类型。更积极的治疗方法如全身化疗通常会导致更严重的不良反应。在纳入的研究中,CR率范围为0%至83%(中位数31%),ORR范围为0%至88%(中位数47%)。5项试验评估了单独或联合的PUVA治疗,总结如下。病灶内IFN-α与PUVA联合使用与单独使用PUVA相比,在24至52周的CR方面可能几乎没有差异(风险比(RR)1.07,95%置信区间(CI)0.87至1.31;2项试验;122名参与者;低确定性证据)。未测量常见不良事件和ORR。一项小型交叉试验发现,每月一次的ECP治疗6个月可能不如每周两次的PUVA治疗3个月有效,PUVA治疗后8名参与者中有2名达到CR,8名参与者中有6名达到ORR,而ECP治疗后无CR或ORR(极低确定性证据)。一些参与者在PUVA治疗后报告了轻微恶心,但未给出具体数据。ECP组有一名参与者因低血压退出。然而,由于证据确定性极低,我们不确定结果。一项比较贝沙罗汀加PUVA与单独使用PUVA长达16周的试验报告,贝沙罗汀加PUVA组有1例光敏反应,而单独使用PUVA组无(87名参与者;低确定性证据)。贝沙罗汀加PUVA与单独使用PUVA在CR(RR 1.41,95% CI 0.71至2.80)和ORR(RR 0.94,95% CI 0.61至1.44)方面可能几乎没有差异(93名参与者;低确定性证据)。一项比较皮下注射IFN-α联合阿维A或PUVA长达48周或直至CR的试验表明,在常见的IFN-α类流感样症状不良反应方面可能几乎没有差异(RR 1.32,95% CI 0.92至1.88;82名参与者)。与IFN-α和PUVA相比,IFN-α和阿维A的CR可能较低(RR 0.54,95% CI 0.35至0.84;82名参与者)(两个结局:低确定性证据)。该试验未测量ORR。一项比较PUVA维持治疗与无维持治疗的试验,在已经达到CR的参与者中进行,确实报告了常见不良反应。然而,分布情况不可评估。CR和OR无法评估。治疗选择的范围意味着罕见的不良反应因此在各种器官中发生。
缺乏高确定性证据来支持MF治疗的决策。由于设计上存在实质性异质性、数据缺失、样本量小以及方法学质量低,基于纳入的RCT无法可靠地确定这些干预措施的相对安全性和疗效。PUVA通常被推荐为MF的一线治疗方法,我们未找到证据对这一推荐提出质疑。没有证据支持在接受PUVA治疗的人群中使用病灶内IFN-α或贝沙罗汀,也没有证据支持使用阿维A或ECP治疗MF。未来的试验应将治疗方法与作为当前护理标准的PUVA的安全性和疗效进行比较,并应测量生活质量和常见不良反应。
