Thiboutot Diane M, Fleischer Alan B, Del Rosso James Q, Rich Phoebe
Pennsylvania State University College of Medicine, Hershey, PA, USA.
J Drugs Dermatol. 2009 Jul;8(7):639-48.
This two-phase, multicenter study was undertaken to examine the safety and efficacy of combination therapy with oral doxycycline and topical azelaic acid (AzA) 15% gel in moderate-to-severe papulopustular rosacea and to determine the effect of subsequent maintenance monotherapy with AzA 15% gel alone. In the initial open-label, non-randomized phase of the study, subjects (n=172) received topical AzA 15% gel and oral doxycycline (100 mg), both twice daily, for < or = 12 weeks. In the second, double-blind study phase, subjects who had initially undergone at least four weeks of combination treatment in phase 1 and who achieved > or = 75% inflammatory lesion count reduction (n=136) were randomized to receive either AzA 15% gel or its vehicle twice daily for an additional 24 weeks. Assessments of efficacy were obtained at four-week intervals throughout both phases of the study and included change in inflammatory lesion count, investigator global assessment (IGA) of rosacea severity, and separate assessments of erythema and telangiectasia severity. At the last visit for each phase of the study, the investigator and participant each rated overall improvement, with the participant rating cosmetic acceptability and the investigator rating treatment as "success" or "failure" based on IGA score. During the second phase of the trial, the rate of relapse -- defined as either a 50% deterioration in the lesion count improvement from phase 1, an increase in erythema intolerable to the subject or maintenance therapy failure as judged by the investigator and/or the subject -- was obtained. Safety assessments were conducted for both phases of the study and included analysis of adverse events (AEs) and a rating of cutaneous tolerability by the subject. By week 12 of the open-label phase of the study, 81.4% of subjects had reached a 75% or greater reduction in inflammatory lesion count, and 64% of patients achieved treatment success. During the second study phase (maintenance phase), AzA 15% gel consistently provided a better maintenance response than vehicle, with maintenance of remission in 75% of patients over the six-month duration of the maintenance phase. Additionally AzA 15% gel showed a statistically significantly lower deterioration in absolute inflammatory lesion counts than did vehicle after 8, 16, 20 and 24 weeks of maintenance therapy. No serious treatment-related AEs were encountered in the study, and 98.5% of subjects were satisfied with the local tolerability of both AzA gel and vehicle.
这项两阶段、多中心研究旨在考察口服多西环素与外用15%壬二酸(AzA)凝胶联合治疗中重度丘疹脓疱型玫瑰痤疮的安全性和有效性,并确定随后单独使用15% AzA凝胶维持单药治疗的效果。在研究的初始开放标签、非随机阶段,受试者(n = 172)接受外用15% AzA凝胶和口服多西环素(100 mg),均每日两次,持续≤12周。在第二个双盲研究阶段,在第1阶段最初接受至少4周联合治疗且炎症性皮损计数减少≥75%的受试者(n = 136)被随机分组,接受15% AzA凝胶或其赋形剂,每日两次,持续额外24周。在研究的两个阶段中,每隔4周进行一次疗效评估,评估内容包括炎症性皮损计数的变化、研究者对玫瑰痤疮严重程度的整体评估(IGA)以及对红斑和毛细血管扩张严重程度的单独评估。在研究的每个阶段的最后一次访视时,研究者和受试者分别对总体改善情况进行评分,受试者对美容可接受性进行评分,研究者根据IGA评分将治疗评定为“成功”或“失败”。在试验的第二阶段,获得复发率——定义为与第1阶段相比皮损计数改善恶化50%、受试者难以耐受的红斑增加或研究者和/或受试者判断维持治疗失败。对研究的两个阶段均进行了安全性评估,包括不良事件(AE)分析和受试者对皮肤耐受性的评分。在研究的开放标签阶段的第12周时,81.4%的受试者炎症性皮损计数减少了75%或更多,64%的患者治疗成功。在第二个研究阶段(维持阶段),15% AzA凝胶始终比赋形剂提供更好的维持反应,在维持阶段的6个月期间,75%的患者维持缓解。此外,在维持治疗8、16、20和24周后,15% AzA凝胶的绝对炎症性皮损计数恶化在统计学上显著低于赋形剂。在研究中未遇到严重的治疗相关AE,98.5%的受试者对AzA凝胶和赋形剂的局部耐受性感到满意。
