Corneal fibrosis: From in vitro models to current and upcoming drug and gene medicines

IF 15.2 1区 医学 Q1 PHARMACOLOGY & PHARMACY
Laura Trujillo Cubillo, Mehmet Gurdal, Dimitrios I. Zeugolis
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引用次数: 0

Abstract

Fibrotic diseases are characterised by myofibroblast differentiation, uncontrolled pathological extracellular matrix accumulation, tissue contraction, scar formation and, ultimately tissue / organ dysfunction. The cornea, the transparent tissue located on the anterior chamber of the eye, is extremely susceptible to fibrotic diseases, which cause loss of corneal transparency and are often associated with blindness. Although topical corticosteroids and antimetabolites are extensively used in the management of corneal fibrosis, they are associated with glaucoma, cataract formation, corneoscleral melting and infection, imposing the need of far more effective therapies. Herein, we summarise and discuss shortfalls and recent advances in in vitro models (e.g. transforming growth factor-β (TGF-β) / ascorbic acid / interleukin (IL) induced) and drug (e.g. TGF-β inhibitors, epigenetic modulators) and gene (e.g. gene editing, gene silencing) therapeutic strategies in the corneal fibrosis context. Emerging therapeutical agents (e.g. neutralising antibodies, ligand traps, receptor kinase inhibitors, antisense oligonucleotides) that have shown promise in clinical setting but have not yet assessed in corneal fibrosis context are also discussed.

Abstract Image

角膜纤维化:从体外模型到当前和未来的药物和基因药物
纤维化疾病的特点是肌成纤维细胞分化、病理细胞外基质不受控制地堆积、组织收缩、疤痕形成,最终导致组织/器官功能障碍。角膜是位于眼球前房的透明组织,极易受到纤维化疾病的影响,导致角膜失去透明度,并常常伴有失明。虽然外用皮质类固醇和抗代谢药物被广泛用于治疗角膜纤维化,但它们与青光眼、白内障形成、角膜巩膜融化和感染有关,因此需要更有效的疗法。在此,我们总结并讨论了角膜纤维化体外模型(如转化生长因子-β(TGF-β)/抗坏血酸/白细胞介素(IL)诱导)、药物(如TGF-β抑制剂、表观遗传调节剂)和基因(如基因编辑、基因沉默)治疗策略的不足之处和最新进展。此外,还讨论了在临床环境中显示出前景但尚未在角膜纤维化背景下进行评估的新兴治疗药物(如中和抗体、配体陷阱、受体激酶抑制剂、反义寡核苷酸)。
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来源期刊
CiteScore
28.10
自引率
5.00%
发文量
294
审稿时长
15.1 weeks
期刊介绍: The aim of the Journal is to provide a forum for the critical analysis of advanced drug and gene delivery systems and their applications in human and veterinary medicine. The Journal has a broad scope, covering the key issues for effective drug and gene delivery, from administration to site-specific delivery. In general, the Journal publishes review articles in a Theme Issue format. Each Theme Issue provides a comprehensive and critical examination of current and emerging research on the design and development of advanced drug and gene delivery systems and their application to experimental and clinical therapeutics. The goal is to illustrate the pivotal role of a multidisciplinary approach to modern drug delivery, encompassing the application of sound biological and physicochemical principles to the engineering of drug delivery systems to meet the therapeutic need at hand. Importantly the Editorial Team of ADDR asks that the authors effectively window the extensive volume of literature, pick the important contributions and explain their importance, produce a forward looking identification of the challenges facing the field and produce a Conclusions section with expert recommendations to address the issues.
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