局部应用环孢素 0.05%停药后干眼减速的可逆性。

Reversibility of dry eye deceleration after topical cyclosporine 0.05% withdrawal.

机构信息

Lakeside Eye Group, SC, Chicago, Illinois 60601, USA.

出版信息

J Ocul Pharmacol Ther. 2011 Dec;27(6):603-9. doi: 10.1089/jop.2011.0073. Epub 2011 Oct 14.

DOI:10.1089/jop.2011.0073

PMID:21999340

Abstract

PURPOSE

To assess the reversibility of clinical benefits of cyclosporine 0.05% (Restasis(®); Allergan, Inc., Irvine, CA) therapy and the therapeutic gain after its delayed use by switching treatment modalities in patients with dry eyes who completed a 1-year course of therapy with artificial tears (Refresh Endura(®); Allergan, Inc., Irvine, CA) or cyclosporine 0.05%.

METHODS

This was a single-center, prospective, investigator-masked, longitudinal extension trial. Patients who had been treated with cyclosporine 0.05% in the first year of study were randomized in a 2:1 ratio to either cyclosporine 0.05% (Cs-Cs; n=20) or artificial tears (Cs-At; n=8), and those who had been originally randomized to artificial tears were switched to cyclosporine 0.05% (At-Cs; n=20) in the second year of study. Patients received study drugs twice daily for 12 months. Disease severity was assessed according to the International Task Force consensus guideline at months 0 and 12. Signs and symptoms were evaluated at baseline (month 0) and months 4, 8, and 12.

RESULTS

At baseline, most patients with Cs-Cs and Cs-At (>90%) had level 2 disease severity, whereas almost half of the patients with At-Cs had level 3 disease severity. At month 12, a significantly higher percentage of patients with Cs-Cs and At-Cs than patients with Cs-At had the same or lower disease severity (P<0.001); whereas half of patients with Cs-At, compared with patients with no Cs-Cs and At-Cs, had disease progression at month 12. Throughout the study, dry eye signs and symptoms continuously improved in patients with Cs-Cs and At-Cs, whereas they constantly worsened in patients with Cs-At. At month 12, patients with Cs-Cs and At-Cs had significantly greater mean percentage improvement from baseline than did patients with Cs-At in Schirmer test scores, tear breakup time, Oxford staining scores, Ocular Surface Disease Index scores, and conjunctival goblet cell density (P<0.001). Overall, sign and symptom scores of patients with At-Cs did not improve as much as they did for patients with Cs-Cs.

CONCLUSIONS

Cyclosporine 0.05% withdrawal led to disease progression, thus indicating the necessity for maintenance therapy. Earlier treatment with cyclosporine 0.05% may result in improved outcomes.

摘要

目的

评估环孢素 0.05%（Restasis®；艾尔建公司，欧文，CA）治疗干眼症患者的临床获益的逆转以及在使用人工泪液（Refresh Endura®；艾尔建公司，欧文，CA）或环孢素 0.05% 治疗 1 年后延迟使用时的治疗增益。

方法

这是一项单中心、前瞻性、研究者设盲、纵向扩展试验。在研究的第一年接受环孢素 0.05%治疗的患者，按照 2:1 的比例随机分为环孢素 0.05%（Cs-Cs；n=20）或人工泪液（Cs-At；n=8）组，而最初随机分配到人工泪液组的患者在研究的第二年转换为环孢素 0.05%（At-Cs；n=20）。患者接受研究药物每日 2 次，持续 12 个月。根据国际专家组共识指南，在第 0 个月和第 12 个月评估疾病严重程度。在基线（第 0 个月）和第 4、8 和 12 个月评估体征和症状。

结果

在基线时，大多数 Cs-Cs 和 Cs-At 患者（>90%）的疾病严重程度为 2 级，而几乎一半的 At-Cs 患者的疾病严重程度为 3 级。在第 12 个月时，与 Cs-At 患者相比，Cs-Cs 和 At-Cs 患者的疾病严重程度相同或更低的比例显著更高（P<0.001）；而一半的 Cs-At 患者与没有 Cs-Cs 和 At-Cs 的患者相比，在第 12 个月时疾病进展。在整个研究过程中，Cs-Cs 和 At-Cs 患者的干眼体征和症状持续改善，而 Cs-At 患者的体征和症状持续恶化。在第 12 个月时，与 Cs-At 患者相比，Cs-Cs 和 At-Cs 患者的 Schirmer 测试评分、泪膜破裂时间、牛津染色评分、眼表疾病指数评分和结膜杯状细胞密度的平均百分比改善均显著更大（P<0.001）。总体而言，与 Cs-Cs 患者相比，Cs-At 患者的体征和症状评分改善程度较低。