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Efficacy of Intravenous Immunoglobulin Monotherapy in Patients with Cutaneous Lupus Erythematosus: Results of Proof-of-Concept Study

机译:皮肤红斑狼疮患者静脉注射免疫球蛋白单一疗法的疗效:概念验证研究的结果

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摘要

Cutaneous lupus erythematosus (CLE) is a chronic inflammatory autoimmune skin disease. Evidence-based therapy for CLE is lacking in the most part. Intravenous immunoglobulin (IVIg) is being increasingly utilized as off-label therapy for a variety of autoimmune and inflammatory conditions, especially in dermatology. The usefulness of IVIg in CLE is not well established. The goal of the present study was to obtain the proof-of-concept evidence that IVIg can control acute CLE and thus replace current systemic immunosuppressive therapy that causes severe side effects and adverse reactions. Sixteen patients who tried and failed various systemic treatments for CLE were screened and consented to use IVIg as a monotherapy. The IVIg was administered at 500 mg/kg/day on 4 consecutive days up to a total of 2 g/kg/month for 3 months, and the subjects were monitored for additional 6 months off any drug for a possible relapse. The cumulative results revealed an overall improvement, as evinced by a decrease of both objective and subjective measures of disease activity. The most sensitive and specific objective and subjective instruments for assessment of the therapeutic effect of IVIg were CLASI-A (Cutaneous Lupus Erythematosus Disease Area and Severity Index) measuring disease activity and Skindex-29 scores, respectively. The CLASI-A score dropped down from the initial value taken as 100%, and remained in the range of approximately 70% until the last visit. Three patients (18.8%) had a temporary flare of CLE symptoms but recovered within a month from the relapse. No serious side effects and adverse reactions occurred. Thus, IVIg monotherapy in CLE allowed to achieve: i) rapid and persistent decreased in disease activity; ii) steady improvement of patients’ quality of life assessed by Skindex-29; iii) low relapse rate; and iv) mild nature and short duration of relapses. Since healing was maintained for months after IVIg treatment, it is possible that the IVIgtriggered molecular events mediating the therapeutic action of IVIg that continued to unfold after the end of therapy.
机译:皮肤红斑狼疮(CLE)是一种慢性炎性自身免疫性皮肤病。大部分缺乏基于证据的CLE治疗。静脉免疫球蛋白(IVIg)越来越多地被用作各种自身免疫和炎性疾病(尤其是皮肤病学)的标记外疗法。 IVIg在CLE中的用处尚不充分。本研究的目的是获得概念性证据,证明IVIg可以控制急性CLE,从而替代目前引起严重副作用和不良反应的全身免疫抑制疗法。筛选了尝试和失败各种CLE全身疗法的16名患者,并同意使用IVIg作为单一疗法。连续4天每天以500 mg / kg /天的剂量施用IVIg,总共3个月共2 g / kg /月,并且监测受试者停药6个月以上是否可能复发。累积结果显示总体改善,疾病活动的客观和主观衡量指标均下降。评估IVIg治疗效果的最敏感,最具体,最客观的工具是分别测量疾病活动度和Skindex-29评分的CLASI-A(红斑狼疮疾病面积和严重性指数)。 CLASI-A得分从最初的100%下降,直到最后一次访视一直保持在大约70%的范围内。三名患者(18.8%)出现了短暂的CLE症状,但在复发后一个月内康复。没有严重的副作用和不良反应发生。因此,在CLE中使用IVIg单一疗法可实现:i)疾病活动迅速而持续地减少; ii)由Skindex-29评估的患者生活质量的稳步提高; iii)复发率低; iv)性质温和,复发时间短。由于在IVIg治疗后维持了几个月的愈合,因此IVIgtriggered分子事件可能介导IVIg的治疗作用,并在治疗结束后继续发展。

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