干眼症患者对局部肿瘤坏死因子 α 拮抗剂利卡明单抗 (OCS-02) 反应的药物基因组学分析

IF 1.9 3区 医学 Q2 OPHTHALMOLOGY Cornea Pub Date : 2024-10-01 Epub Date: 2024-02-28 DOI:10.1097/ICO.0000000000003510
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引用次数: 0

摘要

目的:本研究旨在评估DED患者对外用眼部肿瘤坏死因子α(TNFα)抑制剂利卡明利单抗反应的药物基因组学:在一项随机、载体对照的2期研究中,患有DED且在使用人工泪液治疗后仍有严重眼部不适的成年人接受了为期6周的利卡明利单抗或载体治疗。评估反应的标准是治疗第29天时全球眼部不适评分与基线相比的变化。药物基因组学分析是该研究的一项前瞻性探索目标。研究人员测定了结膜上皮细胞中 TNFα、白细胞介素 (IL) 1β 和 IL8 的 mRNA 表达。采用混合模型重复测量分析评估了SNPs与利卡明单抗反应之间的关系:结果:TNFR1基因中的SNP rs1800693对利卡敏利单抗的反应有显著影响(P < 0.0001,初始关联测试);其他测试的SNP均无影响。与 CT 或 TT 基因型相比,rs1800693 的 CC 基因型对利卡明利单抗的反应更大:CC、CT 和 TT 基因型患者从基线到第 29 天全球眼部不适评分的 LS 平均变化分别为 -29.5、-0.09 和 -3.90(P < 0.0001)。在接受药物治疗的患者中未观察到明显效果。3/4的利卡明利马单抗治疗的 CC 基因型患者的病情较基线有所改善。CC基因型患者结膜上皮细胞的TNFα、IL1β和IL8 mRNA水平比基线有所下降,而CT或TT基因型患者则没有下降。在接受车辆治疗的参与者中,未观察到基因型间 mRNA 水平的差异:rs1800693的CC基因型在DED患者中比较常见,它与对利卡明单抗的反应以及治疗期间眼表面细胞中炎症细胞因子基因表达的减少密切相关。据我们所知,这项研究是首次对治疗 DED 的药物基因组学进行研究。
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Pharmacogenomic Analysis of Response to Topical Tumor Necrosis Factor α Antagonist Licaminlimab (OCS-02) in Dry Eye Disease [RETRACTED].

Purpose: The purpose of this study was to evaluate the pharmacogenomics of response to topical ocular tumor necrosis factor α (TNFα) inhibitor licaminlimab in patients with DED.

Methods: Three single-nucleotide polymorphisms (SNPs) associated with Sjögren syndrome, 3 in the TNFα gene and 1 in the TNF receptor 1 (TNFR1) gene, were assessed for association with response to licaminlimab in participants from a randomized, vehicle-controlled, Phase 2 study in which adults with DED and severe ocular discomfort persisting despite treatment with artificial tears received licaminlimab or vehicle for 6 weeks. Response was assessed for change from baseline in Global Ocular Discomfort score at Day 29 of treatment. The pharmacogenomic analysis was a prospectively specified exploratory objective of the study. mRNA expression for TNFα, interleukin (IL) 1β, and IL8 in conjunctival epithelium cells was determined. The relationship between SNPs and response to licaminlimab was assessed using a mixed model repeated measures analysis.

Results: SNP rs1800693 in the TNFR1 gene showed a significant effect on response to licaminlimab ( P < 0.0001, initial association test); no effect was seen for any of the other SNPs tested. The CC genotype of rs1800693 was associated with much greater response to licaminlimab than the CT or TT genotypes: LS mean changes from baseline to Day 29 in Global Ocular Discomfort score were -29.5, -0.09, and -3.90, in patients with the CC, CT, and TT genotypes, respectively ( P < 0.0001). No significant effect was observed in vehicle-treated patients. Improvements from baseline were seen in 3/4 licaminlimab-treated participants with the CC genotype. Conjunctival epithelium cell levels of mRNA for TNFα, IL1β, and IL8 decreased from baseline in participants with the CC genotype, but not with the CT or TT genotypes. Between-genotype differences in mRNA levels were not observed in participants receiving vehicle.

Conclusions: The CC genotype of rs1800693, relatively common in patients with DED, was strongly associated with response to licaminlimab and decreased inflammatory cytokine gene expression in ocular surface cells during treatment. This study is one of the first to our knowledge to investigate pharmacogenomics in the treatment of DED.

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来源期刊
Cornea
Cornea 医学-眼科学
CiteScore
5.20
自引率
10.70%
发文量
354
审稿时长
3-6 weeks
期刊介绍: For corneal specialists and for all general ophthalmologists with an interest in this exciting subspecialty, Cornea brings together the latest clinical and basic research on the cornea and the anterior segment of the eye. Each volume is peer-reviewed by Cornea''s board of world-renowned experts and fully indexed in archival format. Your subscription brings you the latest developments in your field and a growing library of valuable professional references. Sponsored by The Cornea Society which was founded as the Castroviejo Cornea Society in 1975.
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