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Primary Mechanisms of Thymosin ?24 Repair Activity in Dry Eye Disorders and Other Tissue Injuries

机译:胸腺素?24修复活动在干眼症和其他组织损伤中的主要机制

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Dry eye disorders are becoming more common due to many causes, including an aging population, increased pollution, and postrefractive surgery. Current treatments include artificial tears; gels; lubricants; tear duct plugs; and anti-inflammatory agents such as steroids, doxycycline, and cyclosporine. For more severe forms of the disease, serum tears and scleral contact lenses are employed. Despite these therapies, successful resolution of the problem is limited because none of these treatments fully addresses the underlying causes of dry eye to promote ocular surface repair. Thymosin ?24 (T?24), a small, naturally occurring protein, promotes complete and faster corneal healing than saline alone or prescription agents (doxycycline and cyclosporine) in various animal models of eye injury. In human trials, it improves both the signs and symptoms of moderate to severe dry eye with effects lasting beyond the treatment period. This review will cover the multiple activities of T?24 on cell migration, inflammation, apoptosis, cytoprotection, and gene expression with a focus on mechanisms of cell migration, including laminin-332 synthesis and degradation, that account for this paradigm-shifting potential new treatment for dry eye disorders. We will also speculate on additional mechanisms that might promote eye repair based on data from other tissue injury models. Such studies provide the rationale for use of T?24 in other types of eye disorders beyond dry eye. Finally, we will identify the gaps in our knowledge and propose future research avenues.
机译:由于许多原因,包括人口老龄化,污染增加和屈光后手术,干眼症正变得越来越普遍。目前的治疗方法包括人工泪液;凝胶润滑剂泪管塞;以及抗炎药,例如类固醇,强力霉素和环孢霉素。对于更严重的疾病形式,使用血清泪液和巩膜接触镜。尽管有这些疗法,但成功解决该问题的方法受到限制,因为这些疗法均不能完全解决干眼症促进眼表修复的根本原因。在各种动物眼损伤模型中,胸腺素β24(Tβ24)是一种天然的小蛋白质,与单独使用盐水或处方药(强力霉素和环孢菌素)相比,可促进角膜完全完整和更快地愈合。在人体试验中,它可以改善中度至重度干眼症的症状和体征,其作用持续超过治疗期。这篇综述将涵盖T?24在细胞迁移,炎症,凋亡,细胞保护和基因表达方面的多种活性,重点是细胞迁移的机制,包括层粘连蛋白-332的合成和降解,这些是新的范式转移潜力。干眼症的治疗。我们还将基于其他组织损伤模型的数据,推测可能促进眼睛修复的其他机制。这些研究为在干眼以外的其他类型的眼部疾病中使用T?24提供了理论依据。最后,我们将找出我们的知识差距,并提出未来的研究途径。

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