Altered retinoid metabolism gene expression in chronic Stevens-Johnson syndrome

维甲酸 维甲酸 视黄醇X受体α 孤儿受体 视黄醇X受体 结膜 医学 维甲酸受体 维甲酸 受体 RAR相关孤儿受体γ 视黄醇X受体γ 视黄醇X受体β 病理 内分泌学 分子生物学 免疫学 内科学 生物 核受体 生物化学 免疫系统 基因 转录因子 FOXP3型
作者
Gurumurthy Srividya,Narayanasamy Angayarkanni,Geetha Iyer,Bhaskar Srinivasan,Shweta Agarwal
出处
期刊:British Journal of Ophthalmology [BMJ]
卷期号:103 (8): 1015-1023 被引量:9
标识
DOI:10.1136/bjophthalmol-2018-312849
摘要

Background Stevens-Johnson syndrome (SJS), a blistering disorder of the skin and mucous membrane, leads to ocular morbidity in >60% of cases. Retinoids are vital micronutrients for vision, regulating corneal and conjunctival cell proliferation, differentiation and immune function. This prospective case–control study probed for alterations in retinoid metabolism by evaluating retinoic acid receptor signalling in the conjunctival cells of patients with SJS. Methods Imprints were collected from the bulbar conjunctiva of patients with chronic SJS. The gene expression of retinoic acid receptors, namely, RXRA, RARA, RARG, RORA; the fibrosis marker TGFβ and its receptor TGFβRII ; the transcription factors PPAR-γ, STRA6 and Stat3 ; the enzymes aldehyde dehydrogenase ( ALDH1a1 ), alpha-1 antitrypsin ( A1AT ); and the Cyp genes Cyp26a1 and Cyp26b1 were assessed by quantitative PCR in patients with SJS pre-mucous (n = 34) and post-mucous membrane graft (MMG) intervention (n=19) in comparison with age-matched/sex-matched healthy controls (n=20). Western blot analysis of ALDH1a1, RARA and RARG were done in the conjunctival imprint cells. Results The transcript levels of ALDH1a1, RXRA, RORA, STRA6, Cyp26a1 and Cyp26b1 were decreased around 4, 26, 17, 129, 9 and 8 folds, respectively, and RARA, RARG, PPAR-γ, TGFβ, TGFβRII were increased by 12, 15, 51, 16 and 87 folds, respectively, in SJS conjunctiva at the pre-MMG stage. The changes in RORA, Cyp26a1, Cyp26b1, RARA and Stat3 were statistically significant (p<0.05). Changes in protein expression of ALDH1a1, RARA and RARG supported the gene expression changes. Conclusions The study provides the first experimental insight into the role of retinoid metabolism in the ocular sequelae of chronic SJS.

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