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Tight binding of proteins to membranes from older human cells

机译:蛋白质与老年人细胞膜的紧密结合

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摘要

The lens is an ideal model system for the study of macromolecular aging and its consequences for cellular function, since there is no turnover of lens fibre cells. To examine biochemical processes that take place in the lens and that may also occur in other long-lived cells, membranes were isolated from defined regions of human lenses that are synthesised at different times during life, and assayed for the presence of tightly bound cytosolic proteins using quantitative iTRAQ proteomics technology. A majority of lens beta crystallins and all gamma crystallins became increasingly membrane bound with age, however, the chaperone proteins alpha A and alpha B crystallin, as well as the thermally-stable protein, βB2 crystallin, did not. Other proteins such as brain-associated signal protein 1 and paralemmin 1 became less tightly bound in the older regions of the lens. It is evident that protein–membrane interactions change significantly with age. Selected proteins that were formerly cytosolic become increasingly tightly bound to cell membranes with age and are not removed even by treatment with 7 M urea. It is likely that such processes reflect polypeptide denaturation over time and the untoward binding of proteins to membranes may alter membrane properties and contribute to impairment of communication between older cells.
机译:晶状体是研究大分子老化及其对细胞功能后果的理想模型系统,因为没有晶状体纤维细胞的更新。为了检查晶状体中发生的以及也可能在其他长寿细胞中发生的生化过程,从人晶状体的定义区域中分离了膜,这些区域在生命中的不同时间合成,并分析是否存在紧密结合的胞质蛋白使用定量iTRAQ蛋白质组学技术。随着年龄的增长,大多数晶状体β晶状体蛋白和所有γ晶状体蛋白都越来越与膜结合,但是,伴侣蛋白αA和αB晶状体蛋白以及热稳定蛋白βB2晶状体蛋白却没有。其他蛋白质,例如与大脑相关的信号蛋白1和Paralemmin 1,在晶状体的较旧区域中的结合变得不太紧密。显然,蛋白质与膜的相互作用随着年龄的增长而发生显着变化。随着年龄的增长,以前为胞质的选定蛋白质与细胞膜的结合越来越紧密,即使通过7 M尿素处理也无法去除。这些过程可能反映了多肽随时间的变性,蛋白质与膜的不良结合可能会改变膜的性质,并导致较老细胞之间的通讯受损。

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