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体外角膜内皮伤口闭合。表皮生长因子和/或吲哚美辛的作用。

Corneal endothelial wound closure in vitro. Effects of EGF and/or indomethacin.

作者信息

Joyce N C, Matkin E D, Neufeld A H

机构信息

Ophthalmic Pharmacology Unit, Eye Research Institute, Boston, Massachusetts 02114.

出版信息

Invest Ophthalmol Vis Sci. 1989 Jul;30(7):1548-59.

PMID:2787301
Abstract

In response to stress, the corneal endothelium must maintain or region its barrier function. To study cellular responses of the corneal endothelium, our laboratory has developed an in vitro model of rabbit corneal endothelial wound closure. When cells are free to divide, a 3 mm diameter wound closes within 4 days. 5-fluorouracil added to these cultures does not affect the cellular morphology or ultrastructure, but does inhibit cell division. In the presence of 5-fluorouracil, wounds close in approximately 7 days. These conditions mimic the amitotic state and general behavior of adult human corneal endothelium in vivo. Using this model, we studied the effects of epidermal growth factor (EGF) and/or indomethacin treatment on corneal endothelial wound closure in mitotically competent and inhibited cultures. EGF appeared to stimulate migration, whereas indomethacin appeared to enhance cell spreading in response to wounding, particularly in mitotically inhibited cultures. Treatment with the above agents at the time of wounding had little effect on wound closure rates, but did affect closure patterns. In contrast, pretreatment of cultures, particularly with indomethacin, significantly accelerated closure in mitotically inhibited cultures. In the presence of indomethacin, wounds closed in 3-4 days compared to 7-8 days for controls. These results indicate that the response of corneal endothelial cells to wounding can be pharmacologically manipulated, and perhaps accelerated, and suggest that the treatment of the endothelium with nonsteroidal anti-inflammatory drugs or EGF-like growth factors may be clinically useful.

摘要

作为对压力的反应,角膜内皮必须维持或恢复其屏障功能。为了研究角膜内皮的细胞反应,我们实验室建立了兔角膜内皮伤口闭合的体外模型。当细胞能够自由分裂时,一个直径3毫米的伤口在4天内愈合。向这些培养物中添加5-氟尿嘧啶不会影响细胞形态或超微结构,但会抑制细胞分裂。在5-氟尿嘧啶存在的情况下,伤口大约在7天内愈合。这些条件模拟了成年人类角膜内皮在体内的无丝分裂状态和一般行为。利用这个模型,我们研究了表皮生长因子(EGF)和/或吲哚美辛处理对有丝分裂活性正常和受抑制的培养物中角膜内皮伤口闭合的影响。EGF似乎能刺激迁移,而吲哚美辛似乎能促进受伤后的细胞铺展,特别是在有丝分裂受抑制的培养物中。在受伤时用上述药物处理对伤口闭合率影响不大,但会影响闭合模式。相比之下,对培养物进行预处理,特别是用吲哚美辛预处理,能显著加速有丝分裂受抑制的培养物中的伤口闭合。在吲哚美辛存在的情况下,伤口在3-4天内愈合,而对照组则需要7-8天。这些结果表明,角膜内皮细胞对伤口的反应可以通过药理学手段进行调控,甚至可能加速,这表明用非甾体抗炎药或EGF样生长因子治疗内皮可能具有临床应用价值。

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