0.1% 他扎罗汀乳膏治疗光损伤的疗效：一项为期12个月的多中心随机试验。

Efficacy of 0.1% tazarotene cream for the treatment of photodamage: a 12-month multicenter, randomized trial.

作者信息

Phillips Tania J, Gottlieb Alice B, Leyden James J, Lowe Nicholas J, Lew-Kaya Deborah A, Sefton John, Walker Patricia S, Gibson John R

机构信息

Boston University School of Medicine, Boston, MA 02118, USA.

出版信息

Arch Dermatol. 2002 Nov;138(11):1486-93. doi: 10.1001/archderm.138.11.1486.

DOI:10.1001/archderm.138.11.1486

PMID:12437455

Abstract

OBJECTIVE

To determine the efficacy and safety of 0.1% tazarotene cream for the treatment of photodamage.

DESIGN

A 24-week multicenter, double-blind, randomized, vehicle-controlled intervention study followed by a 28-week open-label extension.

SETTING

Ambulatory patients in private and institutional practice.

PATIENTS

Of 563 patients with facial photodamage, 91% and 86% completed the double-blind and open-label phases, respectively. In the double-blind phase, 20 of 283 tazarotene-treated patients and 1 of 280 vehicle-treated patients discontinued treatment owing to adverse events.

INTERVENTION

Once-daily application of 0.1% tazarotene cream or nonmedicated vehicle cream to the face for 24 weeks. Then, all continuing patients received treatment with 0.1% tazarotene cream for another 28 weeks.

MAIN OUTCOME MEASURES

Primarily, fine wrinkling and mottled hyperpigmentation. Also, lentigines, elastosis, pore size, irregular depigmentation, tactile roughness, coarse wrinkling, telangiectasia, actinic keratoses, overall integrated assessment of photodamage, global response to treatment, patients' overall assessment of photodamage, and plasma levels of tazarotenic acid.

RESULTS

Compared with the vehicle, at week 24 tazarotene resulted in a significantly greater incidence of patients achieving treatment success (>or=50% global improvement) and at least a 1-grade improvement in fine wrinkling, mottled hyperpigmentation, lentigines, elastosis, pore size, irregular depigmentation, tactile roughness, coarse wrinkling, and the overall integrated assessment of photodamage (P<.01). Additional clinical improvement occurred with continued tazarotene treatment and had not plateaued by week 52. Plasma tazarotenic acid concentrations did not exceed 0.71 ng/mL.

CONCLUSIONS

Once-daily applications of 0.1% tazarotene cream significantly reduced multiple signs of photodamage. Plasma levels of tazarotenic acid remained below those of endogenous retinoids.

摘要

目的

确定0.1%他扎罗汀乳膏治疗光损伤的疗效和安全性。

设计

一项为期24周的多中心、双盲、随机、赋形剂对照干预研究，随后进行为期28周的开放标签延长期研究。

地点

私人诊所和机构诊所的门诊患者。

患者

563例面部光损伤患者中，分别有91%和86%完成了双盲期和开放标签期研究。在双盲期，283例接受他扎罗汀治疗的患者中有20例、280例接受赋形剂治疗的患者中有1例因不良事件而中断治疗。

干预措施

每天一次将0.1%他扎罗汀乳膏或无药赋形剂乳膏涂抹于面部，持续24周。然后，所有继续治疗的患者再接受28周的0.1%他扎罗汀乳膏治疗。

主要观察指标

主要为细纹和斑驳状色素沉着。此外，还包括雀斑、弹性组织变性、毛孔大小、不规则色素脱失、触觉粗糙度、粗皱纹、毛细血管扩张、光化性角化病、光损伤的整体综合评估、对治疗的总体反应、患者对光损伤的总体评估以及他扎罗汀酸的血浆水平。

结果

与赋形剂相比，在第24周时，他扎罗汀使治疗成功（全球改善≥50%）的患者发生率显著更高，并且在细纹、斑驳状色素沉着、雀斑、弹性组织变性、毛孔大小、不规则色素脱失、触觉粗糙度、粗皱纹以及光损伤的整体综合评估方面至少有1级改善（P<0.01）。继续使用他扎罗汀治疗可带来额外的临床改善，至第52周时仍未达到平台期。血浆他扎罗汀酸浓度未超过0.71 ng/mL。