Effects of LDLR variants rs5928, rs750518671 and rs879254797 on protein structure and functional activity in HepG2 cells transfected with CRISPR/Cas9 constructs

Effects of LDLR variants rs5928, rs750518671 and rs879254797 on protein structure and functional activity in HepG2 cells transfected with CRISPR/Cas9 constructs

•LDLR missense variants (p.C184Y, p.G373D, p.G549D, p.V797L, p.R814Q and p.V827I) were identified in FH patients.•· p.C184Y, p.G373D and p.G549D altered protein stability and disturbed LDLR intramolecular interactions.•·p.V797L slightly reduced protein stability and p.R814Q potentially disrupted rec...

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Veröffentlicht in:Gene 2024-01, Vol.890, p.147821-147821, Article 147821
Hauptverfasser: Mori, Augusto Akira, Malaquias, Vanessa Barbosa, Bonjour, Kennedy, Ferreira, Glaucio Monteiro, Bortolin, Raul Hernandes, Borges, Jéssica Bassani, Oliveira, Victor Fernandes de, Gonçalves, Rodrigo Marques, Faludi, Andre Arpad, Bastos, Gisele Monteiro, Thurow, Helena, Sampaio, Marcelo Ferraz, Ciconelli, Rozana Mesquita, Cury, Adriano Namo, Fajardo, Cristina Moreno, Hirata, Rosario Dominguez Crespo, Hirata, Mario Hiroyuki
Format: Artikel
Sprache:eng
Schlagworte:
atherosclerosis
computer simulation
confocal microscopy
cost effectiveness
CRISPR
CRISPR-Cas systems
energy
Familial hypercholesterolemia
flow cytometry
Functional analyses
gene frequency
genes
genetic disorders
hypercholesterolemia
LDLR
lipid composition
low density lipoprotein cholesterol
pathogenicity
prediction
protein structure
risk
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Zusammenfassung:•LDLR missense variants (p.C184Y, p.G373D, p.G549D, p.V797L, p.R814Q and p.V827I) were identified in FH patients.•· p.C184Y, p.G373D and p.G549D altered protein stability and disturbed LDLR intramolecular interactions.•·p.V797L slightly reduced protein stability and p.R814Q potentially disrupted receptor anchoring.•·p.G373D, p.V767L and p.R814Q reduced LDLR expression and activity in CRISPR/cas9-transfected HepG2 cells.•Knowledge about the effects of LDLR missense variants contributes to improving the management of FH. Familial Hypercholesterolemia (FH) is a genetic disorder associated with premature atherosclerosis and increased risk of cardiovascular diseases. LDLR deleterious mutations are associated with FH, however the role of some missense variants in FH pathogenicity remains to be elucidated. This study explored the predictive impact of LDLR missense variants on protein structure and investigated their functional effects on LDLR expression in HepG2 cells transfected with CRISPR/Cas9 constructs. FH (n = 287) and non-FH patients (n = 45) were selected, and lipid profile was obtained from medical records. LDLR variants were identified using an exon-targeted gene sequencing strategy, considering its cost-effective to increase accuracy in the identification step of the most likely FH-related variants in a less laborious process. LDLR variants were selected based on conflicting pathogenicity results found in Clinvar, in silico prediction tools, affected LDLR domains, and less common variants considering minor allele frequency A, p.C184Y), rs879254797 (c.1118G>A, p.G373D), rs28941776 (c.1646G>A, p.G549D), rs750518671 (c.2389G>C, p.V797L), rs5928 (c.2441G>A, p.R814Q) and rs137853964 (c.2479G>A, p.V827I) were selected for molecular docking analysis. The p.C184Y exhibited a favorable energy change for protein stability due to its interaction with EGF-A/EGF-B regions; p.G373D and p.G549D displayed intermediate energy changes; and p.R814Q and p.V827I showed smaller energy changes. The results of functional assays showed that
ISSN:0378-1119
1879-0038
DOI:10.1016/j.gene.2023.147821