APOLIPOPROTEIN-E PHENOTYPING BY ISOELECTRIC-FOCUSING IN IMMOBILIZED PH GRADIENTS AND SILVER STAINING

被引:11
|
作者
CARTIER, R [1 ]
SASSOLAS, A [1 ]
机构
[1] NEUROCHIRURG PIERRE WERTHEIMER,F-69394 LYONS 03,FRANCE
来源
ELECTROPHORESIS | 1992年 / 13卷 / 04期
关键词
D O I
10.1002/elps.1150130151
中图分类号
Q5 [生物化学];
学科分类号
071010 ; 081704 ;
摘要
A simple and high resolution procedure of apoprotein E (apo E) phenotyping by isoelectric focusing with immobilized pH gradients and silver staining is described. This method needs delipidated very low density lipoproteins (isolated from 1 mL of serum) but obviates immunoblotting as well as neuraminidase treatment in routine applications because the sialylated forms are clearly separated. Immunoblotting (with polyclonal and monoclonal anti-apo E antiserum), cysteamine and neuraminidase treatment, and pI markers allowed the localization of three main alleles, xi-2, xi-3, xi-4 and the detection of variants or rare alleles (6/450 determinations). The serum amyloid A (SAA) apolipoproteins (SAA1, SAA2) could be characterized unequivocally (especially with E3 and E4). Silver staining proved more sensitive than Coomassie Brilliant Blue and needs only 5-mu-g of protein in the sample. The results of 403 normo-or hyperlipidemic patients are shown. In the group of 191 normolipidemic patients (cholesterol < 6.40 mmol/L triglycerides < 2 mmol/L), the relative frequency of the xi-3 allele (0.83) is higher than in other reports on Caucasians (about 0.77) whereas the xi-4 allele is lower. As previously described, we find a high frequency of the 4/3 phenotype in hypercholesterolemia and 3/2 in hypertriglyceridemia. The high frequency of the E2/E2 phenotype, usually associated with hyperlipidemia, and variants in complex hypertriglyceridemia makes the apo E phenotyping necessary in many cases of dyslipidemias.
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页码:252 / 257
页数:6
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