Next-generation sequencing to confirm clinical familial hypercholesterolemia.

High-Throughput Nucleotide Sequencing Humans Hyperlipoproteinemia Type II / diagnosis Phenotype Proprotein Convertase 9 / genetics Receptors, LDL / genetics
APOB LDLR PCSK9 DLCN Familial hypercholesterolemia MedPed cholesterol lipid metabolism mutation next-generation sequencing

Journal

European journal of preventive cardiology
ISSN: 2047-4881
Titre abrégé: Eur J Prev Cardiol
Pays: England
ID NLM: 101564430

Informations de publication

Date de publication:
23 07 2021
Historique:
received: 13 05 2020
accepted: 28 06 2020
entrez: 23 7 2021
pubmed: 24 7 2021
medline: 15 12 2021
Statut: ppublish

Résumé

Familial hypercholesterolemia is characterised by high low-density lipoprotein-cholesterol levels and is caused by a pathogenic variant in LDLR, APOB or PCSK9. We investigated which proportion of suspected familial hypercholesterolemia patients was genetically confirmed, and whether this has changed over the past 20 years in The Netherlands. Targeted next-generation sequencing of 27 genes involved in lipid metabolism was performed in patients with low-density lipoprotein-cholesterol levels greater than 5 mmol/L who were referred to our centre between May 2016 and July 2018. The proportion of patients carrying likely pathogenic or pathogenic variants in LDLR, APOB or PCSK9, or the minor familial hypercholesterolemia genes LDLRAP1, ABCG5, ABCG8, LIPA and APOE were investigated. This was compared with the yield of Sanger sequencing between 1999 and 2016. A total of 227 out of the 1528 referred patients (14.9%) were heterozygous carriers of a pathogenic variant in LDLR (80.2%), APOB (14.5%) or PCSK9 (5.3%). More than 50% of patients with a Dutch Lipid Clinic Network score of 'probable' or 'definite' familial hypercholesterolemia were familial hypercholesterolemia mutation-positive; 4.8% of the familial hypercholesterolemia mutation-negative patients carried a variant in one of the minor familial hypercholesterolemia genes. The mutation detection rate has decreased over the past two decades, especially in younger patients in which it dropped from 45% in 1999 to 30% in 2018. A rare pathogenic variant in LDLR, APOB or PCSK9 was identified in 14.9% of suspected familial hypercholesterolemia patients and this rate has decreased in the past two decades. Stringent use of clinical criteria algorithms is warranted to increase this yield. Variants in the minor familial hypercholesterolemia genes provide a possible explanation for the familial hypercholesterolemia phenotype in a minority of patients.

Sections du résumé

BACKGROUND
Familial hypercholesterolemia is characterised by high low-density lipoprotein-cholesterol levels and is caused by a pathogenic variant in LDLR, APOB or PCSK9. We investigated which proportion of suspected familial hypercholesterolemia patients was genetically confirmed, and whether this has changed over the past 20 years in The Netherlands.
METHODS
Targeted next-generation sequencing of 27 genes involved in lipid metabolism was performed in patients with low-density lipoprotein-cholesterol levels greater than 5 mmol/L who were referred to our centre between May 2016 and July 2018. The proportion of patients carrying likely pathogenic or pathogenic variants in LDLR, APOB or PCSK9, or the minor familial hypercholesterolemia genes LDLRAP1, ABCG5, ABCG8, LIPA and APOE were investigated. This was compared with the yield of Sanger sequencing between 1999 and 2016.
RESULTS
A total of 227 out of the 1528 referred patients (14.9%) were heterozygous carriers of a pathogenic variant in LDLR (80.2%), APOB (14.5%) or PCSK9 (5.3%). More than 50% of patients with a Dutch Lipid Clinic Network score of 'probable' or 'definite' familial hypercholesterolemia were familial hypercholesterolemia mutation-positive; 4.8% of the familial hypercholesterolemia mutation-negative patients carried a variant in one of the minor familial hypercholesterolemia genes. The mutation detection rate has decreased over the past two decades, especially in younger patients in which it dropped from 45% in 1999 to 30% in 2018.
CONCLUSIONS
A rare pathogenic variant in LDLR, APOB or PCSK9 was identified in 14.9% of suspected familial hypercholesterolemia patients and this rate has decreased in the past two decades. Stringent use of clinical criteria algorithms is warranted to increase this yield. Variants in the minor familial hypercholesterolemia genes provide a possible explanation for the familial hypercholesterolemia phenotype in a minority of patients.

Identifiants

DOI: 10.1093/eurjpc/zwaa451 PMID: 34298557
pubmed: 34298557
pii: 6327116
doi: 10.1093/eurjpc/zwaa451
doi:

Substances chimiques

Receptors, LDL 0
PCSK9 protein, human EC 3.4.21.-
Proprotein Convertase 9 EC 3.4.21.-

Types de publication

Journal Article Research Support, Non-U.S. Gov't

Langues

eng

Sous-ensembles de citation

IM

Pagination

875-883

Commentaires et corrections

Type : CommentIn

Informations de copyright

© The Author(s) 2020. Published by Oxford University Press on behalf of the European Society of Cardiology.

Auteurs

Laurens F Reeskamp (LF)

Department of Vascular Medicine, University of Amsterdam, The Netherlands.

Tycho R Tromp (TR)

Department of Vascular Medicine, University of Amsterdam, The Netherlands.

Joep C Defesche (JC)

Department of Clinical Genetics, University of Amsterdam, The Netherlands.

Aldo Grefhorst (A)

Department of Experimental Vascular Medicine, University of Amsterdam, The Netherlands.

Erik S G Stroes (ESG)

Department of Vascular Medicine, University of Amsterdam, The Netherlands.

G Kees Hovingh (GK)

Department of Vascular Medicine, University of Amsterdam, The Netherlands.

Linda Zuurbier (L)

Department of Clinical Genetics, University of Amsterdam, The Netherlands.

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Classifications MeSH

questionsmedicales.fr Techniques d'investigation Techniques génétiques Analyse de séquence Séquençage nucléotidique à haut débit Next-generation sequencing to confirm clinical...
questionsmedicales.fr Eucaryotes Animaux Chordés Vertébrés Mammifères Eutheria Primates Haplorhini Catarrhini Hominidae Humains Next-generation sequencing to confirm clinical...
questionsmedicales.fr Maladies métaboliques et nutritionnelles Maladies métaboliques Erreurs innées du métabolisme Erreurs innées du métabolisme lipidique Hyperlipoprotéinémie de type II Next-generation sequencing to confirm clinical...
questionsmedicales.fr Phénomènes génétiques Phénotype Next-generation sequencing to confirm clinical...
questionsmedicales.fr Enzymes et coenzymes Enzymes Hydrolases Peptide hydrolases Protéases à sérine Serine endopeptidases Proprotéine convertase 9 Next-generation sequencing to confirm clinical...
questionsmedicales.fr Acides aminés, peptides et protéines Protéines Protéines membranaires Récepteurs de surface cellulaire Récepteurs aux lipoprotéines Récepteurs aux lipoprotéines LDL Next-generation sequencing to confirm clinical...