Refinement of Variant Selection for the LDL Cholesterol Genetic Risk Score in the Diagnosis of the Polygenic Form of Clinical Familial Hypercholesterolemia and Replication in Samples from 6 Countries-Reference-Cited by-同舟云学术

Refinement of Variant Selection for the LDL Cholesterol Genetic Risk Score in the Diagnosis of the Polygenic Form of Clinical Familial Hypercholesterolemia and Replication in Samples from 6 Countries

Published:2015-01-01 Issue:1 Volume:61 Page:231-238
ISSN:0009-9147
Container-title:Clinical Chemistry
language:en
Short-container-title:

Author:

Futema Marta¹,Shah Sonia²³,Cooper Jackie A¹,Li KaWah¹,Whittall Ros A¹,Sharifi Mahtab¹,Goldberg Olivia¹,Drogari Euridiki⁴,Mollaki Vasiliki⁴,Wiegman Albert⁵,Defesche Joep⁶,D'Agostino Maria N⁷⁸,D'Angelo Antonietta⁷⁸,Rubba Paolo⁹,Fortunato Giuliana⁷⁸,Waluś-Miarka Małgorzata¹⁰,Hegele Robert A¹¹,Aderayo Bamimore Mary¹¹,Durst Ronen¹²,Leitersdorf Eran¹²,Mulder Monique T¹³,Roeters van Lennep Jeanine E¹³,Sijbrands Eric J G¹³,Whittaker John C¹⁴¹⁵,Talmud Philippa J¹,Humphries Steve E¹

Affiliation:

1. Centre for Cardiovascular Genetics, British Heart Foundation Laboratories, Institute of Cardiovascular Sciences, and

2. UCL Genetics Institute, Department of Genetics, Environment and Evolution, London, University College London, UK

3. Current affiliation: Centre for Neurogenetics and Statistical Genomics, Queensland Brain Institute, University of Queensland, St. Lucia, Brisbane, Australia

4. 1st Department of Pediatrics, Unit of Metabolic Diseases, Choremio Research Laboratory, University of Athens Medical School, “Aghia Sophia” Children's Hospital, Athens, Greece

5. Department of Pediatrics and

6. Department of Vascular Medicine, Academic Medical Center, Amsterdam, The Netherlands

7. CEINGE S.C.a r.l. Advanced Biotechnology, Naples, Italy

8. Department of Molecular Medicine and Medical Biotechnology, University of Naples Federico II, Naples, Italy

9. Department of Clinical Medicine and Surgery, University of Naples Federico II, Naples, Italy

10. Department of Metabolic Diseases and Department of Medical Didactics, Jagiellonian University Medical College, Krakow, Poland

11. Robarts Research Institute, London, Ontario, Canada

12. Center for Research, Prevention and Treatment of Atherosclerosis, Department of Medicine, Cardiology Division, Hadassah Hebrew University Medical Centre, Jerusalem, Israel

13. Departments of Cardiology and Internal Medicine, Erasmus Medical Center, Rotterdam, The Netherlands

14. Department of Non-Communicable Disease Epidemiology, London School of Hygiene and Tropical Medicine, London, UK

15. GlaxoSmithKline Quantitative Sciences, Medicines Research Centre, Stevenage, Hertfordshire, UK

Abstract

Abstract BACKGROUND Familial hypercholesterolemia (FH) is an autosomal-dominant disorder caused by mutations in 1 of 3 genes. In the 60% of patients who are mutation negative, we have recently shown that the clinical phenotype can be associated with an accumulation of common small-effect LDL cholesterol (LDL-C)-raising alleles by use of a 12–single nucleotide polymorphism (12-SNP) score. The aims of the study were to improve the selection of SNPs and replicate the results in additional samples. METHODS We used ROC curves to determine the optimum number of LDL-C SNPs. For replication analysis, we genotyped patients with a clinical diagnosis of FH from 6 countries for 6 LDL-C-associated alleles. We compared the weighted SNP score among patients with no confirmed mutation (FH/M–), those with a mutation (FH/M+), and controls from a UK population sample (WHII). RESULTS Increasing the number of SNPs to 33 did not improve the ability of the score to discriminate between FH/M– and controls, whereas sequential removal of SNPs with smaller effects/lower frequency showed that a weighted score of 6 SNPs performed as well as the 12-SNP score. Metaanalysis of the weighted 6-SNP score, on the basis of polymorphisms in CELSR2 (cadherin, EGF LAG 7-pass G-type receptor 2), APOB (apolipoprotein B), ABCG5/8 [ATP-binding cassette, sub-family G (WHITE), member 5/8], LDLR (low density lipoprotein receptor), and APOE (apolipoprotein E) loci, in the independent FH/M– cohorts showed a consistently higher score in comparison to the WHII population (P < 2.2 × 10−16). Modeling in individuals with a 6-SNP score in the top three-fourths of the score distribution indicated a >95% likelihood of a polygenic explanation of their increased LDL-C. CONCLUSIONS A 6-SNP LDL-C score consistently distinguishes FH/M– patients from healthy individuals. The hypercholesterolemia in 88% of mutation-negative patients is likely to have a polygenic basis.

Funder

Medical Research Council

British Heart Foundation

Health and Safety Executive

Department of Health Research

National Heart, Lung, and Blood Institute

National Institute on Aging

Agency for Health Care Policy and Research

British Heart Foundation BHF

National Institute for Health Research

University College London

Athens University of Economics and Business

Netherlands Heart Foundation

Publisher

Oxford University Press (OUP)

Subject

Biochemistry (medical),Clinical Biochemistry

Link

http://academic.oup.com/clinchem/article-pdf/61/1/231/32640140/clinchem0231.pdf

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