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Journal of Lipid Research, Vol 28, 1364-1370, Copyright © 1987 by Lipid Research, Inc.
A Steinmetz
Human apolipoprotein E (apoE) exists in the population in three common
genetically determined isoforms, apoE-2, E-3, and E-4, that are coded for
by three alleles epsilon-2, epsilon-3 and epsilon-4 at the apoE structural
gene locus resulting in six phenotypes, three homozygotes (E 2/2, E 3/3,
and E 4/4) and three heterozygotes (E 2/3, E 2/4, and E 3/4). A new
procedure is described that allows identification of apoE isoforms and
phenotypes from whole plasma or serum without the need for isolating
apoE-containing lipoproteins or two-dimensional gel electrophoresis of
serum. This rapid method combines cysteamine treatment of apoE in plasma,
separation in parallel of cysteamine- treated and untreated hydrophobic
serum proteins by charge-shift electrophoresis, and isoelectric focusing of
apolipoproteins with immunoblotting. Compared to phenotyping of apoE after
isolation of VLDL, the new procedure agreed in most cases and may be of
special value in detecting apoE mutants that differ in their cysteine
residues or either are spun off during isolation of lipoproteins or cofocus
with other apoproteins and thus escape detection by conventional one-
dimensional techniques. The method provides a simple tool to screen apoE
isoforms that are known to have a major impact on individual plasma
cholesterol levels.
ARTICLES
Phenotyping of human apolipoprotein E from whole blood plasma by immunoblotting
Abteilung Endokrinologie und Stoffwechsel, Philipps-Universitat, Marburg, F. R. G.
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K. von Bergmann, D. Lutjohann, B. Lindenthal, and A. Steinmetz Efficiency of intestinal cholesterol absorption in humans is not related to apoE phenotype J. Lipid Res., January 1, 2003; 44(1): 193 - 197. [Abstract] [Full Text] [PDF] |
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