Genomic Risk Prediction of Coronary Artery Disease in 480,000 Adults

Inouye, Michael; Abraham, Gad; Nelson, Christopher P.; Wood, Angela; Sweeting, Michael; Dudbridge, Frank; Lai, Florence; Kaptoge, Stephen; Brożyńska, Marta; Wang, Tingting; Ye, Shu; Webb, Tom R.; Rutter, Martin K.; Tzoulaki, Ioanna; Patel, Riyaz; Loos, Ruth J.F.; Keavney, Bernard; Hemingway, Harry; Thompson, John R.; Watkins, Hugh; Deloukas, Panos; Angelantonio, Emanuele Di; Butterworth, Adam S.; Danesh, John; Samani, Nilesh J.

doi:10.1016/j.jacc.2018.07.079

Cited by 586 publications

(566 citation statements)

References 21 publications

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“…Our study substantiates the findings by Inouye et al () and Khera et al () showing that GPRS can boost individual risk prediction of common diseases. Here, we come to the conclusion, that at least for prediction of CAD status there is no need to use a sledge‐hammer to crack the nut.…”

Section: Discussionsupporting

confidence: 93%

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Polygenic risk scores outperform machine learning methods in predicting coronary artery disease status

Gola

Erdmann

Müller‐Myhsok

et al. 2020

Genetic Epidemiology

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Coronary artery disease (CAD) is the leading global cause of mortality and has substantial heritability with a polygenic architecture. Recent approaches of risk prediction were based on polygenic risk scores (PRS) not taking possible nonlinear effects into account and restricted in that they focused on genetic loci associated with CAD, only. We benchmarked PRS, (penalized) logistic regression, naïve Bayes (NB), random forests (RF), support vector machines (SVM), and gradient boosting (GB) on a data set of 7,736 CAD cases and 6,774 controls from Germany to identify the algorithms for most accurate classification of CAD status. The final models were tested on an independent data set from Germany (527 CAD cases and 473 controls). We found PRS to be the best algorithm, yielding an area under the receiver operating curve (AUC) of 0.92 (95% CI [0.90, 0.95], 50,633 loci) in the German test data. NB and SVM (AUC ~ 0.81) performed better than RF and GB (AUC ~ 0.75). We conclude that using PRS to predict CAD is superior to machine learning methods.

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Section: Discussionsupporting

confidence: 93%

“…Therefore, a truly external validation in data generated with a different technology, at another time point, in a different population is required to evaluate the absolute classification performance of the models. Interestingly, this is the case also for other published GPRS by Khera et al () and Inouye et al ().…”

Section: Discussionsupporting

confidence: 79%

Polygenic risk scores outperform machine learning methods in predicting coronary artery disease status

Gola

Erdmann

Müller‐Myhsok

et al. 2020

Genetic Epidemiology

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“…It has always been of clinical focus to foresee the risk of heart failure via genetic background characteristics. GRS was used to identify patients with Mendelian and complex disease patterns known as loci for HF risk factors, such as CAD, Cardiometabolic Disease, Blood Pressure and atrial fibrillation . Heart failure has similar or worse prognosis when compared to most cancers .…”

Section: Discussionmentioning

confidence: 99%

“…Genetic risk scores (GRS), which is the sum of risk genes in individuals has been beneficial to primary prevention. Genome‐wide association study (GWAS) studies have identified 73 gene mutation loci for coronary artery disease (CAD), and almost 100 genes were associated with cardiomyopathies (most of which are DCM and HCM), while only few previous studies such as studies on coronary artery disease, and cardiometabolic diseases in cardiovascular disease have shown the use of genomic information in risk prediction.…”

Section: Introductionmentioning

confidence: 99%

Genetic risk scores to predict the prognosis of chronic heart failure patients in Chinese Han

Sun

et al. 2019

J Cellular Molecular Medi

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Chronic heart failure (CHF) has poor prognosis and polygenic heritability, and the genetic risk score (GRS) to predict CHF outcome has not yet been researched comprehensively. In this study, we sought to establish GRS to predict the outcomes of CHF. We re‐analysed the proteomics data of failing human heart and combined them to filter the data of high‐throughput sequencing in 1000 Chinese CHF cohort. Cox hazards models were used based on single nucleotide polymorphisms (SNPs) to estimate the association of GRS with the prognosis of CHF, and to analyse the difference between individual SNPs and tertiles of genetic risk. In the cohort study, GRS encompassing eight SNPs harboured in seven genes were significantly associated with the prognosis of CHF (P = 2.19 × 10−10 after adjustment). GRS was used in stratifying individuals into significantly different CHF risk, with those in the top tertiles of GRS distribution having HR of 3.68 (95% CI: 2.40‐5.65 P = 2.47 × 10−10) compared with those in the bottom. We developed GRS and demonstrated its association with first event of heart failure endpoint. GRS might be used to stratify individuals for CHF prognostic risk and to predict the outcomes of genomic screening as a complement to conventional risk and NT‐proBNP.

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“…[67][68][69] This approach has been shown to predict risk in patients with FH. 67 A different approach is to use a very large number of SNPs with a lower threshold of statistical significance (49 310 SNPs in one study 70 ; 1.7 million in another 71 ). This has also been shown to be valid in patients with familial hypercholesterolaemia.…”

Section: Emergence Of Pcsk9 As a Rare Cause Of Fh: Discovery Of A Nmentioning

confidence: 99%

Widening the spectrum of genetic testing in familial hypercholesterolaemia: Will it translate into better patient and population outcomes?

2019

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Familial hypercholesterolaemia (FH) is caused by pathogenic variants in LDLR, APOB or PCSK9. Impaired low‐density lipoprotein (LDL) receptor function leads to decreased LDL catabolism and premature atherosclerotic cardiovascular disease (ASCVD). Thousands of LDLR variants are known, but assignation of pathogenicity requires accurate phenotyping, family studies and assessment of LDL receptor function. Precise, genetic diagnosis of FH using targeted next generation sequencing allows for optimal treatment, distinguishing FH from pathogenically distinct disorders requiring different treatment. Polygenic hypercholesterolaemia resulting from an accumulation of LDL cholesterol‐raising single nucleotide polymorphisms (SNPs) could also be suspected by this approach. Similarly, ASCVD risk could be estimated by broader sequencing of cholesterol and non‐cholesterol‐related genes. Both of these areas require further research. The clinical management of FH, focusing on the primary or secondary prevention of ASCVD, has been boosted by PCSK9 inhibitor therapy. The efficacy of PCSK9 inhibitors in homozygous FH may be partly predicted by the LDLR variants. While expanded genetic testing in FH is clinically useful in providing an accurate diagnosis and enabling cost‐effective testing of relatives, further research is needed to establish its value in improving clinical outcomes.

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Genomic Risk Prediction of Coronary Artery Disease in 480,000 Adults

Cited by 586 publications

References 21 publications

Polygenic risk scores outperform machine learning methods in predicting coronary artery disease status

Polygenic risk scores outperform machine learning methods in predicting coronary artery disease status

Genetic risk scores to predict the prognosis of chronic heart failure patients in Chinese Han

Widening the spectrum of genetic testing in familial hypercholesterolaemia: Will it translate into better patient and population outcomes?

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