Systemic Treatment with the Janus Kinase Inhibitor Baricitinib in Ocular Chronic Graft-versus-Host Disease

IF 3.2 Q1 OPHTHALMOLOGY Ophthalmology science Pub Date : 2024-09-30 DOI:10.1016/j.xops.2024.100627
Taylor McManus BS, MS , Noa G. Holtzman MD , Aaron Zhao BS , Chantal Cousineau-Krieger MD , Susan Vitale PhD, MHS , Edmond J. FitzGibbon MD , Debbie Payne BS, MBA , Janine Newgen COT , Celestina Igbinosun BSN, RN , Annie P. Im MD , Cody Peer MS, PhD , William Douglas Figg Sr. Pharm D , Edward W. Cowen MD , Jacqueline W. Mays DDS, PhD , Steven Pavletic MD, PhD , M.Teresa Magone MD
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Abstract

Objective

To investigate the effects of oral baricitinib on ocular surface disease (OSD) in patients with chronic graft-versus-host disease (cGVHD).

Design

Prospective phase 1 to 2 single institution trial.

Subjects

Eighteen patients with ocular graft-versus-host-disease (oGVHD) and systemic steroid-refractory cGVHD.

Methods

Oral baricitinib (2 mg and 4 mg) was administered daily for up to 12 months in an intrapatient dose-escalation design. National Institutes of Health (NIH) oGVHD score, vision, corneal Oxford staining (COS), tear break-up time (TBUT), Schirmer I test (ST) without anesthesia, and microliter tear equivalent conversion were assessed at baseline, 6 months (primary efficacy end point), and 12 months if patients remained on the drug.

Main Outcome Measures

Improvement in NIH oGVHD score, COS, TBUT, and ST results in patients with and without conjunctival fibrosis at 6 months.

Results

At 6 months, the NIH oGVHD score significantly improved (P = 0.014) with all OSD parameters also showing improvement, though not statistically significant. COS baseline, 2.17 to 0.95; TBUT baseline, 6.66 to 8.18 seconds, Schirmer I baseline, 3.86 mm (2.6 μl) to 5.56 mm (3.9 μl). For patients continuing treatment at 12 months improvements persisted compared with the baseline but remained statistically nonsignificant. Corneal Oxford staining decreased to 0.94; TBUT increased to 8.95 seconds, and ST improved to 10.19 mm (7.2 μL). Conjunctival fibrosis was present in 39% (n = 7) of the patients at baseline. The greatest improvement was observed in the 11 patients without prior conjunctival fibrosis compared with the baseline: COS 1.84, TBUT 6.32 seconds, ST 4.07 mm (2.1 μl); 6 months: COS 0.25 (P = 0.018), TBUT 8.62 seconds, ST 9.12 mm (5.4 μl); 12 months: COS 0, TBUT 10.29 seconds, ST 16.88 mm (10.6 μl). Vision was stable in all groups. Two patients developed asymptomatic, self-limited conjunctival papillomas, and 1 patient developed uncomplicated bacterial conjunctivitis twice. No dose limiting toxicity was observed. Severe adverse events with hospitalizations for possible drug-related systemic infections occurred in 5 patients.

Conclusions

Systemic baricitinib was well-tolerated, improved NIH oGVHD scores and OSD parameters in patients with oGVHD, with the greatest benefits observed in patients without pre-existing conjunctival fibrosis. Conjunctival fibrosis may affect outcomes and should be considered in patient selection for clinical trials.

Financial Disclosure(s)

Proprietary or commercial disclosure may be found in the Footnotes and Disclosures at the end of this article.
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用 Janus 激酶抑制剂 Baricitinib 对眼部慢性移植物抗宿主病进行全身治疗
目的研究口服巴利昔尼对慢性移植物抗宿主病(cGVHD)患者眼表疾病(OSD)的影响。方法采用患者内剂量递增设计,每天口服巴利昔尼(2 毫克和 4 毫克)长达 12 个月。美国国立卫生研究院(NIH)oGVHD评分、视力、角膜牛津染色(COS)、泪液破裂时间(TBUT)、无麻醉施尔默I试验(ST)和微升泪液当量转换分别在基线、6个月(主要疗效终点)和12个月时进行评估(如果患者继续用药)。结果6个月时,NIH oGVHD评分显著改善(P = 0.014),所有OSD参数也有所改善,但无统计学意义。COS基线从2.17秒降至0.95秒;TBUT基线从6.66秒降至8.18秒;Schirmer I基线从3.86毫米(2.6微升)升至5.56毫米(3.9微升)。与基线相比,继续治疗 12 个月的患者病情仍有改善,但在统计学上仍无显著性。角膜牛津染色降至 0.94;TBUT 增至 8.95 秒,ST 增至 10.19 毫米(7.2 μL)。基线时,39% 的患者(n = 7)出现结膜纤维化。与基线值相比,11 名没有结膜纤维化的患者的病情改善最大:COS 1.84,TBUT 6.32 秒,ST 4.07 毫米(2.1 μl);6 个月:与基线相比:COS 1.84,TBUT 6.32 秒,ST 4.07 毫米(2.1 微升);6 个月:COS 0.25(P = 0.018),TBUT 8.62 秒,ST 9.12 毫米(5.4 微升);12 个月:12 个月:COS 0,TBUT 10.29 秒,ST 16.88 毫米(10.6 μl)。各组患者的视力均保持稳定。两名患者出现了无症状的自限性结膜乳头状瘤,一名患者出现了两次无并发症的细菌性结膜炎。没有观察到限制剂量的毒性。结论系统性巴利昔尼耐受性良好,可改善oGVHD患者的NIH oGVHD评分和OSD参数,无结膜纤维化的患者获益最大。结膜纤维化可能会影响治疗效果,在选择患者进行临床试验时应加以考虑。
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来源期刊
Ophthalmology science
Ophthalmology science Ophthalmology
CiteScore
3.40
自引率
0.00%
发文量
0
审稿时长
89 days
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