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晶状体中钠钾ATP酶的表达、调节及功能

Expression, regulation and function of Na,K-ATPase in the lens.

作者信息

Delamere Nicholas A, Tamiya Shigeo

机构信息

Department of Ophthalmology and Visual Sciences, School of Medicine, Louisville, Kentucky, USA.

出版信息

Prog Retin Eye Res. 2004 Nov;23(6):593-615. doi: 10.1016/j.preteyeres.2004.06.003.

Abstract

Na,K-ATPase is responsible for maintaining the correct concentrations of sodium and potassium in lens cells. Na,K-ATPase activity is different in the two cell types that make up the lens, epithelial cells and fibers; specific activity in the epithelium is higher than in fibers. In some parts of the fiber mass Na,K-ATPase activity is barely detectable. There is a large body of evidence that suggests Na,K-ATPase-mediated ion transport by the epithelium contributes significantly to the regulation of ionic composition in the entire lens. In some species different Na,K-ATPase isoforms are present in epithelium and fibers but in general, fibers and epithelium express a similar amount of Na,K-ATPase protein. Turnover of Na,K-ATPase by protein synthesis may contribute to preservation of high Na,K-ATPase activity in the epithelium. In ageing lens fibers, oxidation, and glycation may decrease Na,K-ATPase activity. Na,K-ATPase activity in lens fibers and epithelium also may be subject to regulation as the result of protein tyrosine phosphorylation. Moreover, activation of G protein-coupled receptors by agonists such as endothelin-1 elicits changes of Na,K-ATPase activity. The asymmetrical distribution of Na,K-ATPase activity in the epithelium and fibers may contribute to ionic currents that flow in and around the lens. Studies on human cataract and experimental cataract in animals reveal changes of Na,K-ATPase activity but no clear pattern is evident. However, there is a convincing link between abnormal elevation of lens sodium and the opacification of the lens cortex that occurs in age-related human cataract.

摘要

钠钾ATP酶负责维持晶状体细胞中钠和钾的正确浓度。钠钾ATP酶活性在构成晶状体的两种细胞类型,即上皮细胞和纤维细胞中有所不同;上皮细胞中的比活性高于纤维细胞。在纤维团块的某些部位,钠钾ATP酶活性几乎检测不到。有大量证据表明,上皮细胞通过钠钾ATP酶介导的离子转运对整个晶状体离子组成的调节有显著贡献。在某些物种中,上皮细胞和纤维细胞中存在不同的钠钾ATP酶同工型,但一般来说,纤维细胞和上皮细胞表达的钠钾ATP酶蛋白量相似。通过蛋白质合成对钠钾ATP酶的更新可能有助于维持上皮细胞中较高的钠钾ATP酶活性。在老化的晶状体纤维中,氧化和糖基化可能会降低钠钾ATP酶活性。晶状体纤维和上皮细胞中的钠钾ATP酶活性也可能因蛋白质酪氨酸磷酸化而受到调节。此外,内皮素-1等激动剂激活G蛋白偶联受体可引起钠钾ATP酶活性的变化。上皮细胞和纤维细胞中钠钾ATP酶活性的不对称分布可能有助于晶状体内部和周围的离子电流。对人类白内障和动物实验性白内障的研究揭示了钠钾ATP酶活性的变化,但没有明显的清晰模式。然而,晶状体钠异常升高与年龄相关性人类白内障中晶状体皮质浑浊之间存在令人信服的联系。

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