Genetic heterogeneity in familial dysbetalipoproteinemia. The E2(lys146—-gln) variant results in a dominant mode of inheritance.

Genetic heterogeneity in familial dysbetalipoproteinemia. The E2(lys146—-gln) variant results in a dominant mode of inheritance.

As determined by isoelectric focusing, most patients with familial dysbetalipoproteinemia (FD) exhibit the homozygous apolipoprotein (apo) E2E2 phenotype. Only rarely does FD develop in the more common heterozygous phenotypes E3E2 or E4E2. In fact, only 1 to 4% of the E2E2 homozygotes will develop F...

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Main Authors: M Smit, P de Knijff, E van der Kooij-Meijs, C Groenendijk, AM van den Maagdenberg, JA Gevers Leuven, AF Stalenhoef, PM Stuyt, RR Frants, LM Havekes
Format: Article
Language:English
Published: Elsevier 1990-01-01
Series:Journal of Lipid Research
Online Access:http://www.sciencedirect.com/science/article/pii/S0022227520427592
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spelling doaj-f9489dbda100486a85cd88f2a218192b2021-04-25T04:22:40ZengElsevierJournal of Lipid Research0022-22751990-01-013114553Genetic heterogeneity in familial dysbetalipoproteinemia. The E2(lys146—-gln) variant results in a dominant mode of inheritance.M Smit0P de Knijff1E van der Kooij-Meijs2C Groenendijk3AM van den Maagdenberg4JA Gevers Leuven5AF Stalenhoef6PM Stuyt7RR Frants8LM Havekes9Department of Human Genetics, State University of Leiden, The Netherlands.Department of Human Genetics, State University of Leiden, The Netherlands.Department of Human Genetics, State University of Leiden, The Netherlands.Department of Human Genetics, State University of Leiden, The Netherlands.Department of Human Genetics, State University of Leiden, The Netherlands.Department of Human Genetics, State University of Leiden, The Netherlands.Department of Human Genetics, State University of Leiden, The Netherlands.Department of Human Genetics, State University of Leiden, The Netherlands.Department of Human Genetics, State University of Leiden, The Netherlands.Department of Human Genetics, State University of Leiden, The Netherlands.As determined by isoelectric focusing, most patients with familial dysbetalipoproteinemia (FD) exhibit the homozygous apolipoprotein (apo) E2E2 phenotype. Only rarely does FD develop in the more common heterozygous phenotypes E3E2 or E4E2. In fact, only 1 to 4% of the E2E2 homozygotes will develop FD. We wondered whether this reduced penetrance of FD in E2E2 homozygotes could be due to additional heterogeneity in the APOE*2 allele. In the literature a number of different mutations causing an E2 isoelectric focusing variant have been described. To study the genetic heterogeneity of the APOE gene, hybridization of enzymatically amplified genomic DNA with mutation-specific oligonucleotide probes was applied. All FD patients (n = 40) with the E2E2 phenotype appeared to be homozygous for the common E2(arg158—-cys) mutation. However, all three unrelated patients with the E3E2 phenotype exhibited the rare E2(lys146—-gln) mutation due to an A—-C substitution at nucleotide position 3,847 of the APOE gene. This mutation was not found among normolipidemic individuals with the E2E2 (n = 13) or E3E2 phenotype (n = 120) selected from a random population sample. Family studies of the three probands heterozygous for the E*2(lys146—-gln) allele showed that this rare allele predisposes to FD with high penetrance. We conclude that FD is a genetically heterogeneous disease entity, displaying a recessive mode of inheritance with strongly reduced penetrance in case of the common E2(arg158—-cys) variant and with a dominant mode of inheritance with high penetrance in case of the rare E2(lys146—-gln) mutant. It should be noted that in this dominant form presymptomatic diagnosis is possible.http://www.sciencedirect.com/science/article/pii/S0022227520427592
collection DOAJ
language English
format Article
sources DOAJ
author M Smit
P de Knijff
E van der Kooij-Meijs
C Groenendijk
AM van den Maagdenberg
JA Gevers Leuven
AF Stalenhoef
PM Stuyt
RR Frants
LM Havekes
spellingShingle M Smit
P de Knijff
E van der Kooij-Meijs
C Groenendijk
AM van den Maagdenberg
JA Gevers Leuven
AF Stalenhoef
PM Stuyt
RR Frants
LM Havekes
Genetic heterogeneity in familial dysbetalipoproteinemia. The E2(lys146—-gln) variant results in a dominant mode of inheritance.
Journal of Lipid Research
author_facet M Smit
P de Knijff
E van der Kooij-Meijs
C Groenendijk
AM van den Maagdenberg
JA Gevers Leuven
AF Stalenhoef
PM Stuyt
RR Frants
LM Havekes
author_sort M Smit
title Genetic heterogeneity in familial dysbetalipoproteinemia. The E2(lys146—-gln) variant results in a dominant mode of inheritance.
title_short Genetic heterogeneity in familial dysbetalipoproteinemia. The E2(lys146—-gln) variant results in a dominant mode of inheritance.
title_full Genetic heterogeneity in familial dysbetalipoproteinemia. The E2(lys146—-gln) variant results in a dominant mode of inheritance.
title_fullStr Genetic heterogeneity in familial dysbetalipoproteinemia. The E2(lys146—-gln) variant results in a dominant mode of inheritance.
title_full_unstemmed Genetic heterogeneity in familial dysbetalipoproteinemia. The E2(lys146—-gln) variant results in a dominant mode of inheritance.
title_sort genetic heterogeneity in familial dysbetalipoproteinemia. the e2(lys146—-gln) variant results in a dominant mode of inheritance.
publisher Elsevier
series Journal of Lipid Research
issn 0022-2275
publishDate 1990-01-01
description As determined by isoelectric focusing, most patients with familial dysbetalipoproteinemia (FD) exhibit the homozygous apolipoprotein (apo) E2E2 phenotype. Only rarely does FD develop in the more common heterozygous phenotypes E3E2 or E4E2. In fact, only 1 to 4% of the E2E2 homozygotes will develop FD. We wondered whether this reduced penetrance of FD in E2E2 homozygotes could be due to additional heterogeneity in the APOE*2 allele. In the literature a number of different mutations causing an E2 isoelectric focusing variant have been described. To study the genetic heterogeneity of the APOE gene, hybridization of enzymatically amplified genomic DNA with mutation-specific oligonucleotide probes was applied. All FD patients (n = 40) with the E2E2 phenotype appeared to be homozygous for the common E2(arg158—-cys) mutation. However, all three unrelated patients with the E3E2 phenotype exhibited the rare E2(lys146—-gln) mutation due to an A—-C substitution at nucleotide position 3,847 of the APOE gene. This mutation was not found among normolipidemic individuals with the E2E2 (n = 13) or E3E2 phenotype (n = 120) selected from a random population sample. Family studies of the three probands heterozygous for the E*2(lys146—-gln) allele showed that this rare allele predisposes to FD with high penetrance. We conclude that FD is a genetically heterogeneous disease entity, displaying a recessive mode of inheritance with strongly reduced penetrance in case of the common E2(arg158—-cys) variant and with a dominant mode of inheritance with high penetrance in case of the rare E2(lys146—-gln) mutant. It should be noted that in this dominant form presymptomatic diagnosis is possible.
url http://www.sciencedirect.com/science/article/pii/S0022227520427592
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