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免疫化学证据支持在暴露于4-羟基-2-壬烯醛的蛋白质上形成2-戊基吡咯。

Immunochemical evidence supporting 2-pentylpyrrole formation on proteins exposed to 4-hydroxy-2-nonenal.

作者信息

Sayre L M, Sha W, Xu G, Kaur K, Nadkarni D, Subbanagounder G, Salomon R G

机构信息

Department of Chemistry, Case Western Reserve University, Cleveland, Ohio 44106, USA.

出版信息

Chem Res Toxicol. 1996 Oct-Nov;9(7):1194-201. doi: 10.1021/tx960094j.

Abstract

Previous model studies suggested the formation of lysine-based 2-pentylpyrroles as novel late adduction products formed upon exposure of proteins to the lipid peroxidation product 4-hydroxy-2-nonenal (HNE). Two 2-pentylpyrrole immunogens were prepared, one by treating keyhole limpet hemocyanin (KLH) directly with 4-oxononanal and the other by preformation of 6-(2-pentylpyrrol-1-yl)hexanoic acid from 6-aminocaproic acid and 4-oxononanal, followed by carbodiimide coupling to KLH. Pyrrole content and lysine modification in KLH were assayed independently. Following immunization of rabbits, antibody titer increased and plateaued over a 4 month period. The structural specificity of the IgG fractions of the antisera was evaluated through comprehensive competitive ELISA studies. These antibodies were used to verify the time-dependent appearance of the 2-pentylpyrrole epitope in protein exposed to HNE. Potential advantages of antibodies recognizing "advanced lipid peroxidation end products" over those recognizing "early" HNE adduction products are discussed.

摘要

先前的模型研究表明,在蛋白质暴露于脂质过氧化产物4-羟基-2-壬烯醛(HNE)时,会形成基于赖氨酸的2-戊基吡咯,作为新的晚期加合物产物。制备了两种2-戊基吡咯免疫原,一种是通过将钥孔血蓝蛋白(KLH)直接用4-氧代壬醛处理,另一种是由6-氨基己酸和4-氧代壬醛预先形成6-(2-戊基吡咯-1-基)己酸,然后通过碳二亚胺偶联到KLH上。分别测定了KLH中的吡咯含量和赖氨酸修饰情况。对兔子进行免疫后,抗体滴度在4个月内升高并趋于平稳。通过全面的竞争性ELISA研究评估了抗血清IgG组分的结构特异性。这些抗体用于验证暴露于HNE的蛋白质中2-戊基吡咯表位的时间依赖性出现。讨论了识别“晚期脂质过氧化终产物”的抗体相对于识别“早期”HNE加合物产物的抗体的潜在优势。

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