Targeted sequencing in patients with clinically diagnosed hereditary lipid metabolism disorder and acute coronary syndrome

Author:

Averkova AO1ORCID,Brazhnik VA2ORCID,Speshilov GI3ORCID,Rogozhina AA1ORCID,Koroleva OS1,Zubova EA4,Galyavich AS5ORCID,Tereshenko SN6,Boyeva OI7,Zateyshchikov DA2ORCID

Affiliation:

1. Central State Medical Academy of the Department of Presidential Affairs of the Russian Federation, Moscow

2. Central State Medical Academy of the Department of Presidential Affairs of the Russian Federation, Moscow; Municipal Clinical Hospital No. 51, Moscow

3. Kharkevich Institute for Information Transmission Problems, RAS, Moscow; ReadSense OOO, Troitsk Center for Nanotechnologies of Rusnano Foundation for Nanotechnology Infrastructure and Educational Projects, Moscow

4. Municipal Clinical Hospital No. 51, Moscow

5. Kazan State Medical University, Kazan

6. National Medical Research Center for Cardiology, Moscow

7. Stavropol State Medical University, Stavropol

Abstract

The actual prevalence of genetic variants causing familial hypercholesterolemia (FH) in every population remains unknown. The aim of this work was to determine the spectrum of pathogenic variants in patients with acute coronary syndrome (ACS) and clinically diagnosed FH using targeted sequencing. We selected 38 patients with ACS from the sample of 2,081 participants of two multicenter observational studies (2004–2007; 2014–2016) who had a clinical diagnosis of FH based on the Dutch Lipid Clinic Network score and Simon Broome criteria. The men and women included in the study were ≤ 55 and ≤ 60 years of age, respectively. Molecular genetic screening was done by targeted next-generation sequencing. We started by sequencing 3 genes associated with FH, including LDLR, APOB, and PCSK9. If no relevant variants were detected, the panel was expanded. Of 38 patients, 24 (63.2%) were shown to have mutations that could cause clinical manifestations of FH and premature coronary artery disease. All patients were heterozygous carriers. Mutations were detected in three “classic” genes LDLR, APOB, and PCSK9 associated with FH, as well as in other genes involved in lipid metabolism, such as APOE, ABCA1, ABCG5, ABCG8, LPL, ANGPTL3, and MTTP. Five variants detected in our study sample had not been described previously: the pathogenic p.Val273_Cys313del variant of the LDLR gene, the likely pathogenic p.Arg160His variant in the APOE gene, two variants of uncertain significance p.Glu612Lys and c.*415G>A in the PCSK9 gene, and the mutant variant p.Ala776Ser in the LDLR gene. We conclude that the use of clinical diagnostic criteria in patients with ACS and FH enables identification of carriers of both “classic” mutations associated with FH and rare genetic variants that can be phenotypically expressed as FH.

Publisher

Pirogov Russian National Research Medical University

Subject

General Medicine

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