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转酮醇酶基因在角膜中的表达受环境因素和发育控制事件的影响。

Transketolase gene expression in the cornea is influenced by environmental factors and developmentally controlled events.

作者信息

Sax C M, Kays W T, Salamon C, Chervenak M M, Xu Y S, Piatigorsky J

机构信息

Laboratory of Molecular and Developmental Biology, National Eye Institute, National Institutes of Health, Bethesda, Maryland, 20892-2730, USA.

出版信息

Cornea. 2000 Nov;19(6):833-41. doi: 10.1097/00003226-200011000-00014.

Abstract

PURPOSE

Transketolase (TKT) has been proposed to be a corneal crystallin, and its gene and protein are abundantly expressed in the corneal epithelium of several mammals. A marked up-regulation of TKT gene expression coincides with the time of eyelid opening in the mouse. Here, we examined whether exposure to incident light contributes to the up-regulation of TKT gene expression during cornea maturation.

METHODS

Mice were raised in either standard light/dark cycling conditions or total darkness. In some cases, subcutaneous injections of epidermal growth factor (EGF) were given beginning on the day of birth to induce early eyelid opening. RNA was prepared from the corneas of mothers and pups and subjected to Northern blot analyses. In addition, the relative levels of TKT mRNA and/or enzyme activity were examined in the corneas of human, bovine, rat, chicken, and zebrafish.

RESULTS

TKT mRNA levels were 2.1-fold higher in the corneas of 25-day-old mouse pups ( 12 days after eyelid opening) that had been born and raised in light/dark conditions compared to pups born and raised in total darkness. By contrast, the level of TKT mRNA in the mature corneas of adult mice maintained in the dark for 2-8 weeks did not vary greatly from those of mice maintained in light/dark conditions. Interestingly, TKT mRNA levels in the corneas of dark-raised mice, although reduced, did exhibit the increase characteristically observed before and after eyelid opening. In addition, TKT mRNA levels were elevated fivefold in the corneas of 28-day-old mice raised in darkness and injected with EGF compared to uninjected mice also deprived of light. The EGF-injected mice opened their eyes 3 days early, and their corneal epithelium did not grossly differ from that of control mice. TKT mRNA and/or enzyme activity was found to be much higher in the corneas than in other tissues of humans, bovines, and rats but was extremely low in the corneas of chicken and zebrafish.

CONCLUSION

Our studies suggest that both exposure to incident light and events surrounding the process of eyelid opening play a role in the up-regulation of TKT gene expression observed during corneal maturation in mice. Light appears to play a less important role in the mature cornea in maintaining high levels of TKT gene expression. The low levels of TKT in the cornea of chicken and zebrafish support the notion that TKT acts as a taxon-specific enzyme-crystallin in mammals. The involvement of environmental signals for this putative, mammalian cornea crystallin contrasts with the purely developmental signals involved in the up-regulation of the crystallin genes of the lens.

摘要

目的

转酮醇酶(TKT)被认为是一种角膜晶状体蛋白,其基因和蛋白在多种哺乳动物的角膜上皮中大量表达。TKT基因表达的显著上调与小鼠睁眼时间一致。在此,我们研究了暴露于入射光是否有助于角膜成熟过程中TKT基因表达的上调。

方法

将小鼠饲养在标准的明暗循环条件或完全黑暗环境中。在某些情况下,从出生当天开始皮下注射表皮生长因子(EGF)以诱导早期睁眼。从母鼠和幼鼠的角膜中提取RNA并进行Northern印迹分析。此外,检测了人、牛、大鼠、鸡和斑马鱼角膜中TKT mRNA和/或酶活性的相对水平。

结果

与在完全黑暗环境中出生和饲养的幼鼠相比,在明暗条件下出生和饲养的25日龄小鼠幼崽(睁眼后12天)角膜中的TKT mRNA水平高2.1倍。相比之下,在黑暗中饲养2 - 8周的成年小鼠成熟角膜中TKT mRNA水平与在明暗条件下饲养的小鼠相比变化不大。有趣的是,在黑暗中饲养的小鼠角膜中TKT mRNA水平虽然降低,但确实呈现出在睁眼前后典型观察到的增加。此外,与同样未受光照的未注射小鼠相比,在黑暗中饲养并注射EGF的28日龄小鼠角膜中TKT mRNA水平升高了五倍。注射EGF的小鼠提前3天睁眼,其角膜上皮与对照小鼠相比无明显差异。发现人、牛和大鼠角膜中的TKT mRNA和/或酶活性比其他组织高得多,但在鸡和斑马鱼的角膜中极低。

结论

我们的研究表明,暴露于入射光和睁眼过程周围的事件在小鼠角膜成熟过程中观察到的TKT基因表达上调中均起作用。在维持高水平TKT基因表达方面,光在成熟角膜中似乎起的作用较小。鸡和斑马鱼角膜中TKT水平较低支持了TKT在哺乳动物中作为分类群特异性酶晶状体蛋白的观点。这种假定的哺乳动物角膜晶状体蛋白涉及环境信号,这与晶状体晶状体蛋白基因上调所涉及的纯粹发育信号形成对比。

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