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关于U18666A白内障尿素可溶性多肽的组成与起源

On the composition and origin of the urea-soluble polypeptides of the U18666A cataract.

作者信息

Cenedella R J, Augusteyn R C

机构信息

Department of Biochemistry, Kirksville College of Osteopathic Medicine, MO 63501.

出版信息

Curr Eye Res. 1990 Sep;9(9):805-18. doi: 10.3109/02713689008999553.

Abstract

The composition and origin of the urea soluble polypeptides which accumulate in the U18666A rat-cataract were studied. Chromatography on Sephacryl S-200 in 7.2 M urea separated the USP into 19-20 and 22-26 kDa enriched fractions. The polypeptide composition of these fractions was probed by immunoblotting of IEF and 2-D electrophoresis gels. The cataract USP largely focused at pHs comparable to alpha- and beta-crystallins. Immunoblotting of 2-D gels showed the USP to be composed predominantly of alpha- and beta-derived crystallins; little gamma-polypeptide was detected in the gels. Some of the insoluble alpha-crystallin appeared to be degraded. Changes in the lens WSP which accompanied the increase in USP were also measured. WSP decreased more than USP increased. Decreases in soluble high molecular weight proteins (alpha- plus beta-crystallins) and medium molecular weight proteins (beta-crystallins) were calculated which together could entirely account for the increased USP. An unexpected decrease in the lens soluble low molecular weight proteins (gamma-crystallins) appeared largely due to the selective leakage of gammas from the lens. The protein content of the ocular humors from eyes with cataracts increased 4 fold and contained polypeptides that focused on IEF like gamma-light crystallin and reacted with the gamma-crystallin antiserum. The cause of the protein insolubilization in the U18666A cataract is unknown but could be partially due to increased aggregation of alpha-crystallins secondary to loss of gamma-crystallins from the lens.

摘要

对在U18666A大鼠白内障中积累的尿素可溶性多肽的组成和来源进行了研究。在7.2 M尿素中于Sephacryl S - 200上进行色谱分离,将尿素可溶性多肽(USP)分离为富含19 - 20 kDa和22 - 26 kDa的组分。通过等电聚焦(IEF)和双向电泳凝胶的免疫印迹法探究了这些组分的多肽组成。白内障USP在很大程度上聚焦于与α-和β-晶状体蛋白相当的pH值。双向凝胶的免疫印迹显示USP主要由α-和β-衍生的晶状体蛋白组成;在凝胶中检测到的γ-多肽很少。一些不溶性α-晶状体蛋白似乎发生了降解。还测量了伴随USP增加的晶状体水溶性蛋白(WSP)的变化。WSP的减少幅度大于USP的增加幅度。计算了可溶性高分子量蛋白(α-加β-晶状体蛋白)和中分子量蛋白(β-晶状体蛋白)的减少量,它们加起来可以完全解释USP的增加。晶状体可溶性低分子量蛋白(γ-晶状体蛋白)意外减少,这在很大程度上是由于γ-晶状体蛋白从晶状体中选择性泄漏所致。患有白内障的眼睛房水中的蛋白质含量增加了4倍,并且含有在IEF上聚焦类似γ-轻晶状体蛋白并与γ-晶状体蛋白抗血清反应的多肽。U18666A白内障中蛋白质不溶性化的原因尚不清楚,但可能部分是由于晶状体中γ-晶状体蛋白丢失导致α-晶状体蛋白聚集增加所致。

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