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Autor: Froguel, Philippe

5 záznamů v Medvik Filtry

Článek

Phenome-wide association analysis of LDL-cholesterol lowering genetic variants in PCSK9

Schmidt, Amand F
Autor Schmidt, Amand F Institute of Cardiovascular Science, University College London, 222 Euston Road, London, NW1 2DA, UK. amand.schmidt@ucl.ac.uk. Department of Cardiology, Division Heart & Lungs, University Medical Center Utrecht, Utrecht University, Utrecht, the Netherlands. amand.schmidt@ucl.ac.uk. UCL's BHF Research Accelerator Centre, London, UK. amand.schmidt@ucl.ac.uk
Holmes, Michael V
Autor Holmes, Michael V Medical Research Council Population Health Research Unit, Clinical Trial Service Unit & Epidemiological Studies Unit (CTSU), Nuffield Department of Population Health, University of Oxford, Oxford, UK
Preiss, David
Autor Preiss, David Medical Research Council Population Health Research Unit, Clinical Trial Service Unit & Epidemiological Studies Unit (CTSU), Nuffield Department of Population Health, University of Oxford, Oxford, UK
Swerdlow, Daniel I
Autor Swerdlow, Daniel I Institute of Cardiovascular Science, University College London, 222 Euston Road, London, NW1 2DA, UK. Department of Medicine, Imperial College London, London, UK
Denaxas, Spiros
Autor Denaxas, Spiros UCL's BHF Research Accelerator Centre, London, UK. Health Data Research UK, University College London, 222 Euston Road, London, NW1 2DA, UK. Institute of Health Informatics, University College London, 222 Euston Road, London, NW1 2DA, UK. The Alan Turing Institute, British Library, 96 Euston Rd, London, NW1 2DB, UK
Fatemifar, Ghazaleh
Autor Fatemifar, Ghazaleh UCL's BHF Research Accelerator Centre, London, UK. Health Data Research UK, University College London, 222 Euston Road, London, NW1 2DA, UK. Institute of Health Informatics, University College London, 222 Euston Road, London, NW1 2DA, UK
Faraway, Rupert
Autor Faraway, Rupert Institute of Cardiovascular Science, University College London, 222 Euston Road, London, NW1 2DA, UK
Finan, Chris
Autor Finan, Chris Institute of Cardiovascular Science, University College London, 222 Euston Road, London, NW1 2DA, UK. UCL's BHF Research Accelerator Centre, London, UK
Valentine, Dennis
Autor Valentine, Dennis UCL's BHF Research Accelerator Centre, London, UK. University College London, Farr Institute of Health Informatics, London, UK
Fairhurst-Hunter, Zammy
Autor Fairhurst-Hunter, Zammy Clinical Trial Service Unit & Epidemiological Studies Unit (CTSU), Nuffield Department of Population Health, University of Oxford, Richard Doll Building, Old Road Campus, Roosevelt Drive, Oxford, OX3 7LF, UK

BMC cardiovascular disorders. 2019 ; 19 (1) : 240. [pub] 20191029

BMC Cardiovasc Disord
ISSN 1471-2261
Medvik
Zdroj

BACKGROUND: We characterised the phenotypic consequence of genetic variation at the PCSK9 locus and compared findings with recent trials of pharmacological inhibitors of PCSK9. METHODS: Published and individual participant level data (300,000+ participants) were combined to construct a weighted PCSK9 gene-centric score (GS). Seventeen randomized placebo controlled PCSK9 inhibitor trials were included, providing data on 79,578 participants. Results were scaled to a one mmol/L lower LDL-C concentration. RESULTS: The PCSK9 GS (comprising 4 SNPs) associations with plasma lipid and apolipoprotein levels were consistent in direction with treatment effects. The GS odds ratio (OR) for myocardial infarction (MI) was 0.53 (95% CI 0.42; 0.68), compared to a PCSK9 inhibitor effect of 0.90 (95% CI 0.86; 0.93). For ischemic stroke ORs were 0.84 (95% CI 0.57; 1.22) for the GS, compared to 0.85 (95% CI 0.78; 0.93) in the drug trials. ORs with type 2 diabetes mellitus (T2DM) were 1.29 (95% CI 1.11; 1.50) for the GS, as compared to 1.00 (95% CI 0.96; 1.04) for incident T2DM in PCSK9 inhibitor trials. No genetic associations were observed for cancer, heart failure, atrial fibrillation, chronic obstructive pulmonary disease, or Alzheimer's disease - outcomes for which large-scale trial data were unavailable. CONCLUSIONS: Genetic variation at the PCSK9 locus recapitulates the effects of therapeutic inhibition of PCSK9 on major blood lipid fractions and MI. While indicating an increased risk of T2DM, no other possible safety concerns were shown; although precision was moderate.

Článek

A catalog of genetic loci associated with kidney function from analyses of a million individuals

Nature genetics. 2019 ; 51 (6) : 957-972. [pub] 20190531

Nat Genet
ISSN 1546-1718
Medvik
Zdroj

Chronic kidney disease (CKD) is responsible for a public health burden with multi-systemic complications. Through trans-ancestry meta-analysis of genome-wide association studies of estimated glomerular filtration rate (eGFR) and independent replication (n = 1,046,070), we identified 264 associated loci (166 new). Of these, 147 were likely to be relevant for kidney function on the basis of associations with the alternative kidney function marker blood urea nitrogen (n = 416,178). Pathway and enrichment analyses, including mouse models with renal phenotypes, support the kidney as the main target organ. A genetic risk score for lower eGFR was associated with clinically diagnosed CKD in 452,264 independent individuals. Colocalization analyses of associations with eGFR among 783,978 European-ancestry individuals and gene expression across 46 human tissues, including tubulo-interstitial and glomerular kidney compartments, identified 17 genes differentially expressed in kidney. Fine-mapping highlighted missense driver variants in 11 genes and kidney-specific regulatory variants. These results provide a comprehensive priority list of molecular targets for translational research.

MeSH
běloši MeSH
celogenomová asociační studie MeSH
chronická renální insuficience genetika patofyziologie moč MeSH
fenotyp MeSH
genetická predispozice k nemoci * MeSH
genetické asociační studie metody MeSH
hodnoty glomerulární filtrace MeSH
jednonukleotidový polymorfismus MeSH
kvantitativní znak dědičný * MeSH
lidé MeSH
lokus kvantitativního znaku * MeSH
mapování chromozomů MeSH
typy dědičnosti MeSH
uromodulin moč MeSH
vyšetření funkce ledvin MeSH
Check Tag
lidé MeSH
Publikační typ
časopisecké články MeSH
metaanalýza MeSH
práce podpořená grantem MeSH

Článek

PCSK9 genetic variants and risk of type 2 diabetes: a mendelian randomisation study

The lancet. Diabetes & endocrinology. 2017 ; 5 (2) : 97-105. [pub] 20161129

Lancet Diabetes Endocrinol
ISSN 2213-8595
Medvik
Zdroj

BACKGROUND: Statin treatment and variants in the gene encoding HMG-CoA reductase are associated with reductions in both the concentration of LDL cholesterol and the risk of coronary heart disease, but also with modest hyperglycaemia, increased bodyweight, and modestly increased risk of type 2 diabetes, which in no way offsets their substantial benefits. We sought to investigate the associations of LDL cholesterol-lowering PCSK9 variants with type 2 diabetes and related biomarkers to gauge the likely effects of PCSK9 inhibitors on diabetes risk. METHODS: In this mendelian randomisation study, we used data from cohort studies, randomised controlled trials, case control studies, and genetic consortia to estimate associations of PCSK9 genetic variants with LDL cholesterol, fasting blood glucose, HbA1c, fasting insulin, bodyweight, waist-to-hip ratio, BMI, and risk of type 2 diabetes, using a standardised analysis plan, meta-analyses, and weighted gene-centric scores. FINDINGS: Data were available for more than 550 000 individuals and 51 623 cases of type 2 diabetes. Combined analyses of four independent PCSK9 variants (rs11583680, rs11591147, rs2479409, and rs11206510) scaled to 1 mmol/L lower LDL cholesterol showed associations with increased fasting glucose (0·09 mmol/L, 95% CI 0·02 to 0·15), bodyweight (1·03 kg, 0·24 to 1·82), waist-to-hip ratio (0·006, 0·003 to 0·010), and an odds ratio for type diabetes of 1·29 (1·11 to 1·50). Based on the collected data, we did not identify associations with HbA1c (0·03%, -0·01 to 0·08), fasting insulin (0·00%, -0·06 to 0·07), and BMI (0·11 kg/m2, -0·09 to 0·30). INTERPRETATION: PCSK9 variants associated with lower LDL cholesterol were also associated with circulating higher fasting glucose concentration, bodyweight, and waist-to-hip ratio, and an increased risk of type 2 diabetes. In trials of PCSK9 inhibitor drugs, investigators should carefully assess these safety outcomes and quantify the risks and benefits of PCSK9 inhibitor treatment, as was previously done for statins. FUNDING: British Heart Foundation, and University College London Hospitals NHS Foundation Trust (UCLH) National Institute for Health Research (NIHR) Biomedical Research Centre.

MeSH
diabetes mellitus 2. typu krev diagnóza genetika MeSH
genetická predispozice k nemoci genetika MeSH
genetická variace genetika MeSH
kohortové studie MeSH
krevní glukóza metabolismus MeSH
LDL-cholesterol krev genetika MeSH
lidé MeSH
mendelovská randomizace metody MeSH
proproteinkonvertasa subtilisin/kexin typu 9 genetika MeSH
randomizované kontrolované studie jako téma metody MeSH
studie případů a kontrol MeSH
Check Tag
lidé MeSH
Publikační typ
časopisecké články MeSH

Článek

Familial mild hyperglycemia associated with a novel ABCC8-V84I mutation within three generations

Pediatric diabetes. 2011 ; 12 (3 Pt 2) : 266-9. [pub] 20110109

Pediatr Diabetes
ISSN 1399-5448
Medvik
Zdroj

We present a unique case of a 19-year-old man with a positive family history of persistent mild hyperglycemia and a novel V84I mutation in ABCC8. The proband was initially detected to have fasting hyperglycemia (ranging 6.1-6.4 mmol/L) at the age of 12 years. Increased fasting blood glucose was also subsequently detected in five additional family members (in his twin brother, sister, mother, maternal aunt, and grandfather). The grandfather has been known to have mild diabetes since 30 years and has never been treated. After having excluded a causative mutation in five maturity-onset diabetes of the young genes (MODY1-4 and 6), we identified a novel ABCC8 V84I mutation, which segregated with autosomal dominant transmission of mild hyperglycemia within three generations. This mutation that is located in a conserved area of transmembrane domain TMD0 seems to be a rare cause of clinical phenotype resembling glucokinase-deficient diabetes.

MeSH
ABC transportéry genetika MeSH
dítě MeSH
dominantní geny MeSH
dospělí MeSH
draslíkové kanály dovnitř usměrňující genetika MeSH
hyperglykemie genetika MeSH
lidé středního věku MeSH
lidé MeSH
mladiství MeSH
mladý dospělý MeSH
receptory léků genetika MeSH
Check Tag
dítě MeSH
dospělí MeSH
lidé středního věku MeSH
lidé MeSH
mladiství MeSH
mladý dospělý MeSH
mužské pohlaví MeSH
Publikační typ
časopisecké články MeSH
kazuistiky MeSH
práce podpořená grantem MeSH

Článek

Association of the calpain-10 gene with type 2 diabetes in Europeans: results of pooled and meta-analyses

Molecular genetics and metabolism. 2006 ; 89 (1-2) : 174-184.

Mol Genet Metab
ISSN 1096-7192
Medvik
Zdroj

We conducted pooled and meta-analyses of the association of the calpain-10 gene (CAPN10) polymorphisms SNP-43, Indel-19 and SNP-63 individually and as haplotypes with type 2 diabetes (T2D) in 3237 patients and 2935 controls of European ancestry. In the pooled analyses, the common SNP-43*G allele was associated with modest but statistically significant increased risk of T2D (odds ratio (OR)=1.11 (95% confidence interval (CI), 1.02-1.20), P=0.01). Two haplotype combinations were associated with increased risk of T2D (1-2-1/1-2-1, OR=1.20 (1.03-1.41), P=0.02; and 1-1-2/1-2-1, OR=1.26 (1.01-1.59), P=0.04) and one with decreased risk (1-1-1/2-2-1, OR=0.86 (0.75-0.99), P=0.03). The meta-analysis also showed a significant effect of the 1-2-1/1-2-1 haplogenotype on risk (OR=1.25 (1.05-1.50), P=0.01). However, there was evidence for heterogeneity with respect to this effect (P=0.06). The heterogeneity appeared to be due to data sets in which the cases were selected from samples used in linkage studies of T2D. Using only the population-based case-control samples removed the heterogeneity (P=0.89) and strengthened the evidence for association with T2D in both the pooled (SNP-43*G, OR=1.19 (1.07-1.32), P=0.001; 1-2-1/1-2-1 haplogenotype, OR=1.46 (1.19-1.78), P=0.0003; 1-1-2/1-2-1 haplogenotype, OR=1.52 (1.12-2.06), P=0.007; and 1-1-1/2-2-1 haplogenotype, OR=0.83 (0.70-0.99), P=0.03) and the meta-analysis (SNP-43*G, OR=1.18 (1.05-1.32), P=0.005; 1-2-1/1-2-1 haplogenotype, OR=1.68 (1.33-2.11), P=0.00001). The pooled and meta-analyses as well as the linkage disequilibrium and haplotype diversity studies suggest a role for genetic variation in CAPN10 affecting risk of T2D in Europeans.

MeSH
běloši * genetika MeSH
diabetes mellitus 2. typu * genetika MeSH
haplotypy genetika MeSH
jednonukleotidový polymorfismus * MeSH
kalpain * genetika MeSH
lidé MeSH
vazebná nerovnováha * MeSH
Check Tag
lidé MeSH
Publikační typ
metaanalýza MeSH
multicentrická studie MeSH
práce podpořená grantem MeSH
Research Support, N.I.H., Extramural MeSH

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