评估氨甲环酸口服液、改良克利格曼配方和安慰剂药膏对黄褐斑疗效的随机研究。

IF 1.9 Q3 DERMATOLOGY
Indian Dermatology Online Journal Pub Date : 2024-08-19 eCollection Date: 2024-09-01 DOI:10.4103/idoj.idoj_797_23
S Prathyoosha, K Ananditha, T Narayana Rao, K V T Gopal, P V Krishnam Raju
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引用次数: 0

摘要

背景:尽管有各种治疗方法,但黄褐斑的治疗往往不彻底,复发率很高。本研究旨在评估口服氨甲环酸(TXA)、改良克利格曼配方(MKF)和安慰剂药膏对黄褐斑的疗效和安全性:90 例男女黄褐斑患者分为三组,每组 30 例。黄褐斑的基线严重程度由黄褐斑面积严重程度指数(MASI)评分。A、B、C组患者分别接受口服 TXA 250 毫克,每天两次,每天晚上使用 MKF 霜,每天晚上使用安慰剂霜,共治疗 12 周。4周、8周和12周后计算MASI评分的改善情况。每次就诊时,如果有不良反应,都会记录下来。统计分析采用卡方检验:根据意向治疗分析,12 周后,口服 TXA 组、MKF 组和安慰剂组的 MASI 评分分别降低了 9.94(65.91%)、6.12(54.78%) 和 2.07(17.22%)(P = 0.00)。口服 TXA 组和 MKF 组 12 周后的平均 MASI 评分降低率差异不显著(P = 0.29)。口服 TXA 和 MKB 组的疗效明显高于安慰剂组(P = 0.01 和 P = 0.03)。各组的不良反应均为轻微且有自限性:研究局限性:样本量有限、非盲法设计、未进行皮肤镜评估:结论:口服 TXA 具有极佳的安全性,可作为治疗中重度黄褐斑的较佳选择。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A Randomized Study to Evaluate the Efficacy of Oral Tranexamic Acid, Modified Kligman's Formula, and Placebo Cream in Melasma.

Background: Despite the availability of various treatment modalities, the treatment of melasma is often incomplete, with a high recurrence rate. The present study was undertaken to assess the efficacy and safety of oral tranexamic acid (TXA), modified Kligman's formula (MKF), and a placebo cream in melasma.

Materials and methods: Ninety cases of melasma of both sexes were enrolled, and divided into three groups of 30 patients each. The baseline severity of melasma was graded by Melasma Area Severity Index (MASI) score. Group A, B, and C patients were treated with oral TXA 250 mg twice daily, daily MKF cream at night, and daily placebo cream at night, respectively, for 12 weeks. Improvement in MASI score was calculated after 4, 8, and 12 weeks. At each visit, adverse effects, if any, were noted. Statistical analysis was done using Chi-square test.

Results: Based on intention to treat analysis, at the end of 12 weeks, the reduction in MASI score in oral TXA, MKF, and placebo groups was 9.94(65.91%), 6.12(54.78%), and 2.07(17.22%), respectively (P = 0.00). The difference in reduction of mean MASI scores after 12 weeks between oral TXA group and MKF group was not significant (P = 0.29). The efficacy of oral TXA and MKB was significantly higher than that of the placebo group (P = 0.01 and P = 0.03, respectively). Adverse effects in all groups were mild and self-limiting.

Limitations: A limited sample size, non-blinded design, and absence of dermoscopic evaluation were the study limitations.

Conclusion: In view of its excellent safety profile, oral TXA may be considered as a better option for moderate to severe melasma.

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来源期刊
CiteScore
2.00
自引率
11.80%
发文量
201
审稿时长
49 weeks
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