Department of Dermatology, University of Minnesota Medical School, Minneapolis, MN, USA.
Department of Dermatology, Lothian University Hospitals NHS Trust, Lauriston Building, Edinburgh, UK.
Cochrane Database Syst Rev. 2022 Mar 11;3(3):CD013130. doi: 10.1002/14651858.CD013130.pub2.
Stevens-Johnson syndrome (SJS), toxic epidermal necrolysis (TEN), and SJS/TEN overlap syndrome are rare, severe cutaneous adverse reactions usually triggered by medications. In addition to tertiary-level supportive care, various systemic therapies have been used including glucocorticoids, intravenous immunoglobulins (IVIGs), cyclosporin, N-acetylcysteine, thalidomide, infliximab, etanercept, and plasmapheresis. There is an unmet need to understand the efficacy of these interventions.
To assess the effects of systemic therapies (medicines delivered orally, intramuscularly, or intravenously) for the treatment of SJS, TEN, and SJS/TEN overlap syndrome.
We searched the following databases up to March 2021: the Cochrane Skin Specialised Register, CENTRAL, MEDLINE, and Embase. We also searched five clinical trial registers, the reference lists of all included studies and of key review articles, and a number of drug manufacturer websites. We searched for errata or retractions of included studies.
We included only randomised controlled trials (RCTs) and prospective observational comparative studies of participants of any age with a clinical diagnosis of SJS, TEN, or SJS/TEN overlap syndrome. We included all systemic therapies studied to date and permitted comparisons between each therapy, as well as between therapy and placebo.
We used standard methodological procedures as specified by Cochrane. Our primary outcomes were SJS/TEN-specific mortality and adverse effects leading to discontinuation of SJS/TEN therapy. Secondary outcomes included time to complete re-epithelialisation, intensive care unit length of stay, total hospital length of stay, illness sequelae, and other adverse effects attributed to systemic therapy. We rated the certainty of the evidence for each outcome using GRADE.
We included nine studies with a total of 308 participants (131 males and 155 females) from seven countries. We included two studies in the quantitative meta-analysis. We included three RCTs and six prospective, controlled observational studies. Sample sizes ranged from 10 to 91. Most studies did not report study duration or time to follow-up. Two studies reported a mean SCORe of Toxic Epidermal Necrosis (SCORTEN) of 3 and 1.9. Seven studies did not report SCORTEN, although four of these studies reported average or ranges of body surface area (BSA) (means ranging from 44% to 51%). Two studies were set in burns units, two in dermatology wards, one in an intensive care unit, one in a paediatric ward, and three in unspecified inpatient units. Seven studies reported a mean age, which ranged from 29 to 56 years. Two studies included paediatric participants (23 children). We assessed the results from one of three RCTs as low risk of bias in all domains, one as high, and one as some concerns. We judged the results from all six prospective observational comparative studies to be at a high risk of bias. We downgraded the certainty of the evidence because of serious risk of bias concerns and for imprecision due to small numbers of participants. The interventions assessed included systemic corticosteroids, tumour necrosis factor-alpha (TNF-alpha) inhibitors, cyclosporin, thalidomide, N-acetylcysteine, IVIG, and supportive care. No data were available for the main comparisons of interest as specified in the review protocol: etanercept versus cyclosporin, etanercept versus IVIG, IVIG versus supportive care, IVIG versus cyclosporin, and cyclosporin versus corticosteroids. Corticosteroids versus no corticosteroids It is uncertain if there is any difference between corticosteroids (methylprednisolone 4 mg/kg/day for two more days after fever had subsided and no new lesions had developed) and no corticosteroids on disease-specific mortality (risk ratio (RR) 2.55, 95% confidence interval (CI) 0.72 to 9.03; 2 studies; 56 participants; very low-certainty evidence). Time to complete re-epithelialisation, length of hospital stay, and adverse effects leading to discontinuation of therapy were not reported. IVIG versus no IVIG It is uncertain if there is any difference between IVIG (0.2 to 0.5 g/kg cumulative dose over three days) and no IVIG in risk of disease-specific mortality (RR 0.33, 95% CI 0.04 to 2.91); time to complete re-epithelialisation (mean difference (MD) -2.93 days, 95% CI -4.4 to -1.46); or length of hospital stay (MD -2.00 days, 95% CI -5.81 to 1.81). All results in this comparison were based on one study with 36 participants, and very low-certainty evidence. Adverse effects leading to discontinuation of therapy were not reported. Etanercept (TNF-alpha inhibitor) versus corticosteroids Etanercept (25 mg (50 mg if weight > 65 kg) twice weekly "until skin lesions healed") may reduce disease-specific mortality compared to corticosteroids (intravenous prednisolone 1 to 1.5 mg/kg/day "until skin lesions healed") (RR 0.51, 95% CI 0.16 to 1.63; 1 study; 91 participants; low-certainty evidence); however, the CIs were consistent with possible benefit and possible harm. Serious adverse events, such as sepsis and respiratory failure, were reported in 5 of 48 participants with etanercept and 9 of 43 participants with corticosteroids, but it was not clear if they led to discontinuation of therapy. Time to complete re-epithelialisation and length of hospital stay were not reported. Cyclosporin versus IVIG It is uncertain if there is any difference between cyclosporin (3 mg/kg/day or intravenous 1 mg/kg/day until complete re-epithelialisation, then tapered off (10 mg/day reduction every 48 hours)) and IVIG (continuous infusion 0.75 g/kg/day for 4 days (total dose 3 g/kg) in participants with normal renal function) in risk of disease-specific mortality (RR 0.13, 95% CI 0.02 to 0.98, 1 study; 22 participants; very low-certainty evidence). Time to complete re-epithelialisation, length of hospital stay, and adverse effects leading to discontinuation of therapy were not reported. No studies measured intensive care unit length of stay.
AUTHORS' CONCLUSIONS: When compared to corticosteroids, etanercept may result in mortality reduction. For the following comparisons, the certainty of the evidence for disease-specific mortality is very low: corticosteroids versus no corticosteroids, IVIG versus no IVIG and cyclosporin versus IVIG. There is a need for more multicentric studies, focused on the most important clinical comparisons, to provide reliable answers about the best treatments for SJS/TEN.
Stevens-Johnson 综合征(SJS)、中毒性表皮坏死松解症(TEN)和 SJS/TEN 重叠综合征是罕见的严重皮肤不良反应,通常由药物引发。除了三级支持性护理外,还使用了各种系统疗法,包括糖皮质激素、静脉注射免疫球蛋白(IVIG)、环孢素、N-乙酰半胱氨酸、沙利度胺、英夫利昔单抗、依那西普和血浆置换。了解这些干预措施的疗效存在未满足的需求。
评估治疗 SJS、TEN 和 SJS/TEN 重叠综合征的系统疗法(口服、肌内或静脉给予的药物)的疗效。
我们检索了截至 2021 年 3 月的以下数据库:Cochrane 皮肤专业注册库、CENTRAL、MEDLINE 和 Embase。我们还检索了五个临床试验注册库、所有纳入研究和关键综述文章的参考文献列表,以及一些药物制造商的网站。我们检索了纳入研究的勘误表或撤稿。
我们纳入了所有年龄的 SJS、TEN 或 SJS/TEN 重叠综合征临床诊断参与者的随机对照试验(RCT)和前瞻性观察性比较研究。我们纳入了迄今为止所有的系统疗法,并允许对每种疗法进行比较,以及对每种疗法与安慰剂进行比较。
我们使用 Cochrane 规定的标准方法学程序。我们的主要结局是 SJS/TEN 特异性死亡率和导致 SJS/TEN 治疗中断的不良事件。次要结局包括完全上皮化的时间、重症监护病房住院时间、总住院时间、疾病后遗症和归因于系统治疗的其他不良事件。我们使用 GRADE 对每个结局的证据确定性进行评级。
我们纳入了来自七个国家的九项研究,共 308 名参与者(男性 131 名,女性 155 名)。我们对两项研究进行了定量荟萃分析。我们纳入了三项 RCT 和六项前瞻性、对照观察性研究。样本量从 10 到 91 不等。大多数研究没有报告研究持续时间或随访时间。两项研究报告了 SCORe of Toxic Epidermal Necrosis(SCORTEN)的平均分数为 3 和 1.9。七项研究没有报告 SCORTEN,但其中四项研究报告了平均或范围的体表面积(BSA)(均值范围为 44%至 51%)。两项研究在烧伤病房进行,两项在皮肤科病房进行,一项在重症监护病房进行,一项在儿科病房进行,三项在未指明的住院病房进行。七项研究报告了平均年龄,范围从 29 岁到 56 岁。两项研究包括儿科参与者(23 名儿童)。我们将三项 RCT 中的一项评为所有领域的偏倚风险低,一项评为高,一项评为存在一些担忧。我们将所有六项前瞻性观察性比较研究的结果评为偏倚风险高。由于严重的偏倚风险和参与者数量少导致的精度问题,我们降低了证据的确定性。评估的干预措施包括系统皮质类固醇、肿瘤坏死因子-α(TNF-α)抑制剂、环孢素、沙利度胺、N-乙酰半胱氨酸、IVIG 和支持性护理。由于没有按审查方案规定的主要比较进行数据:依那西普与环孢素、依那西普与 IVIG、IVIG 与支持性护理、IVIG 与环孢素和环孢素与皮质类固醇。皮质类固醇与无皮质类固醇:我们不确定皮质类固醇(发热消退且无新皮损出现后再给予 4 毫克/千克/天甲基泼尼松龙 2 天)与无皮质类固醇之间是否存在任何差异对疾病特异性死亡率(风险比(RR)2.55,95%置信区间(CI)0.72 至 9.03;2 项研究;56 名参与者;极低确定性证据)。完全上皮化的时间、住院时间和导致治疗中断的不良事件未报告。IVIG 与无 IVIG:我们不确定 IVIG(0.2 至 0.5 克/千克累积剂量在三天内)与无 IVIG 之间是否存在任何差异在疾病特异性死亡率风险(RR 0.33,95% CI 0.04 至 2.91);完全上皮化的时间(平均差异(MD)-2.93 天,95% CI -4.4 至 -1.46);或住院时间(MD -2.00 天,95% CI -5.81 至 1.81)。所有这些比较的结果都基于一项涉及 36 名参与者的研究,证据确定性极低。导致治疗中断的不良事件未报告。依那西普(TNF-α 抑制剂)与皮质类固醇:与皮质类固醇(静脉内泼尼松龙 1 至 1.5 毫克/千克/天“直至皮肤病变愈合”)相比,依那西普(每周两次 25 毫克(体重>65 公斤时为 50 毫克))可能降低疾病特异性死亡率(RR 0.51,95% CI 0.16 至 1.63;1 项研究;91 名参与者;低确定性证据);然而,CI 与可能的获益和可能的危害一致。严重不良事件,如败血症和呼吸衰竭,在接受依那西普治疗的 48 名参与者中有 5 例,在接受皮质类固醇治疗的 43 名参与者中有 9 例报告,但尚不清楚它们是否导致治疗中断。完全上皮化的时间和住院时间未报告。环孢素与 IVIG:我们不确定环孢素(3 毫克/千克/天或静脉内 1 毫克/千克/天,直至完全上皮化,然后逐渐减少(每 48 小时减少 10 毫克))与 IVIG(在肾功能正常的参与者中,连续输注 0.75 克/千克/天 4 天(总剂量 3 克/千克))在疾病特异性死亡率风险方面是否存在任何差异(RR 0.13,95% CI 0.02 至 0.98,1 项研究;22 名参与者;非常低确定性证据)。完全上皮化的时间、住院时间和导致治疗中断的不良事件未报告。没有研究测量重症监护病房住院时间。
与皮质类固醇相比,依那西普可能降低死亡率。对于以下比较,疾病特异性死亡率的证据确定性非常低:皮质类固醇与无皮质类固醇、IVIG 与无 IVIG 和环孢素与 IVIG。需要更多的多中心研究,重点关注最重要的临床比较,以提供有关 SJS/TEN 最佳治疗方法的可靠答案。
