甲状腺眼病的单细胞转录组学研究

IF 1 Q4 OPHTHALMOLOGY Taiwan Journal of Ophthalmology Pub Date : 2023-10-20 DOI:10.4103/tjo.tjo-d-23-00096
Sofia Ahsanuddin, Albert Y. Wu
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引用次数: 0

摘要

甲状腺眼病(TED)是一种影响眶后组织的自身免疫性疾病。组织炎症、扩张和纤维化可能导致衰弱的后遗症,如视力下降、眼球运动疼痛、眼球突出和眼睑收缩。目前TED的治疗方式包括全身性糖皮质激素、硫胺、甲巯咪唑、替原单抗、受体阻滞剂和放射性碘;然而,据报道,高达10%-20%的TED患者在停药后复发,20%-30%的患者对主流治疗无反应,原因尚不清楚。在过去的4年里,视觉研究人员利用高通量单细胞RNA测序来阐明单细胞分辨率下驱动TED发病机制的细胞类型多样性和分子机制。这些研究为新的生物标志物和治疗靶点提供了前所未有的见解。这篇及时的综述总结了利用单细胞和单核转录组学数据来表征这种高度复杂的疾病状态的最新突破和新兴机会。我们还概述了该技术的当前挑战和未来应用,以潜在地改善患者的生活质量并促进疾病终点的逆转。
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Single-cell transcriptomics in thyroid eye disease
Abstract Thyroid eye disease (TED) is a poorly understood autoimmune condition affecting the retroorbital tissue. Tissue inflammation, expansion, and fibrosis can potentially lead to debilitating sequelae such as vision loss, painful eye movement, proptosis, and eyelid retraction. Current treatment modalities for TED include systemic glucocorticoids, thioamides, methimazole, teprotumumab, beta-blockers, and radioactive iodine; however, it has been reported that up to 10%–20% of TED patients relapse after treatment withdrawal and 20%–30% are unresponsive to mainstay therapy for reasons that have yet to be more clearly elucidated. In the past 4 years, vision researchers have harnessed high-throughput single-cell RNA sequencing to elucidate the diversity of cell types and molecular mechanisms driving the pathogenesis of TED at single-cell resolution. Such studies have provided unprecedented insight regarding novel biomarkers and therapeutic targets in TED. This timely review summarizes recent breakthroughs and emerging opportunities for using single-cell and single-nuclei transcriptomic data to characterize this highly complex disease state. We also provide an overview of current challenges and future applications of this technology to potentially improve patient quality of life and facilitate reversal of disease endpoints.
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来源期刊
CiteScore
1.80
自引率
9.10%
发文量
68
审稿时长
19 weeks
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