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βH-晶状体蛋白暴露于羟基自由基会增强其现有胺供体和胺受体位点对转谷氨酰胺酶的敏感性。

Exposure of beta H-crystallin to hydroxyl radicals enhances the transglutaminase-susceptibility of its existing amine-donor and amine-acceptor sites.

作者信息

Groenen P J, Seccia M, Smulders R H, Gravela E, Cheeseman K H, Bloemendal H, de Jong W W

机构信息

Department of Biochemistry, University of Nijmegen, The Netherlands.

出版信息

Biochem J. 1993 Oct 15;295 ( Pt 2)(Pt 2):399-404. doi: 10.1042/bj2950399.

Abstract

beta H-crystallin was exposed to radiolytically generated hydroxyl radicals at defined radical concentrations, and its capacity to act as an amine-acceptor substrate and as an amine-donor substrate for transglutaminase were investigated. [14C]Methylamine was used as a probe for labelling amine-acceptor sites; a novel biotinylated hexapeptide was used to label amine-donor sites. The results demonstrate that both primary amine incorporation and hexapeptide incorporation by transglutaminase are considerably increased after oxidative attack on the crystallin. The identity of the labelled subunits was established, and it is shown that, in both cases, this increased incorporation is not due to the production of new substrates, but that the existing incorporation sites become more susceptible. Moreover, using the newly developed probe, we could identify, for the first time, the major crystallin subunits active as amine-donor substrates (both before and after treatment) to be beta B1-, beta A3- and beta A4-crystallin. These data support the proposal that oxidative stress and transglutaminase activity may be jointly involved in the changes found in lens crystallins with age and in the development of cataract.

摘要

将βH-晶状体蛋白暴露于特定自由基浓度下通过辐射分解产生的羟基自由基中,并研究其作为转谷氨酰胺酶的胺受体底物和胺供体底物的能力。使用[14C]甲胺作为标记胺受体位点的探针;一种新型生物素化六肽用于标记胺供体位点。结果表明,在对晶状体蛋白进行氧化攻击后,转谷氨酰胺酶介导的伯胺掺入和六肽掺入均显著增加。确定了标记亚基的身份,结果表明,在这两种情况下,掺入增加并非由于产生了新的底物,而是现有的掺入位点变得更易受影响。此外,使用新开发的探针,我们首次确定,作为胺供体底物的主要晶状体蛋白亚基(处理前后)为βB1-、βA3-和βA4-晶状体蛋白。这些数据支持以下观点:氧化应激和转谷氨酰胺酶活性可能共同参与晶状体蛋白随年龄变化以及白内障形成过程中所发现的变化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3183/1134895/715dcada8b08/biochemj00101-0079-a.jpg

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