A custom next-generation sequencing panel identified pathogenic and possibly pathogenic variants in 57.9% (33 of 57) of pediatric patients with familial hypercholesterolemia.
Cross-Sectional (n=57)
A custom NGS panel successfully identified pathogenic variants in over half of pediatric FH patients, including a novel LDLR mutation, expanding the genetic spectrum of the disease.
The most common form of inherited lipid disorders is familial hypercholesterolemia (FH). It is characterized primarily by high concentrations of the clinical triad of low-density lipoprotein cholesterol, tendon xanthomas and premature CVD. The well-known genetic background are mutations in LDLR, APOB and PCSK9 gene. Causative mutations can be found in 60−80% of definite FH patients and 20−30% of those with possible FH. Their occurrence could be attributed to the activity of minor candidate genes, whose causal mechanism has not been fully discovered. The aim of the conducted study was to identify disease-causing mutations in FH-related and candidate genes in pediatric patients from Poland using next generation sequencing (NGS). An NGS custom panel was designed to cover 21 causative and candidate genes linked to primary dyslipidemia. Recruitment was performed using Simon Broome diagnostic criteria. Targeted next generation sequencing was performed on a MiniSeq sequencer (Illumina, San Diego, CA, USA) using a 2 × 150 bp paired-end read module. Sequencing data analysis revealed pathogenic and possibly pathogenic variants in 33 out of 57 studied children. The affected genes were LDLR, APOB, ABCG5 and LPL. A novel pathogenic 7bp frameshift deletion c. 373₃79delCAGTTCG in the exon 4 of the LDLR gene was found. Our findings are the first to identify the c. 373₃79delCAGTTCG mutation in the LDLR gene. Furthermore, the double heterozygous carrier of frameshift insertion c. 2416dupG in the LDLR gene and missense variant c. 10708C>T in the APOB gene was identified. The c. 2416dupG variant was defined as pathogenic, as confirmed by its cosegregation with hypercholesterolemia in the proband’s family. Although the APOB c. 10708C>T variant was previously detected in hypercholesterolemic patients, our data seem to demonstrate no clinical impact. Two missense variants in the LPL gene associated with elevated triglyceride plasma level (c. 106G>A and c. 953A>G) were also identified. The custom NGS panel proved to be an effective research tool for identifying new causative aberrations in a genetically heterogeneous disease as familial hypercholesterolemia (FH). Our findings expand the spectrum of variants associated with the FH loci and will be of value in genetic counseling among patients with the disease.
Rutkowska et al. (Wed,) conducted a cross-sectional in Familial hypercholesterolemia (n=57). Custom next-generation sequencing (NGS) panel was evaluated on Identification of pathogenic and possibly pathogenic variants. A custom next-generation sequencing panel identified pathogenic and possibly pathogenic variants in 57.9% (33 of 57) of pediatric patients with familial hypercholesterolemia.
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