Maciej Banach, Martyna Fronczek, T. Osadnik, A. Gach, D. Strapagiel, M. Słomka, M. Lejawa, Anna Goc, E. Boniewska-Bernacka, Anna Pańczyszyn, G. Lip, P. Toth, P. Penson, J. Jóźwiak
{"title":"使用多基因风险评分 (PRS) 对 LIPIDOGEN2015 群体进行为期 8 年的随访,根据常见基因变异得出的不良心血管事件风险--研究设计与方法。","authors":"Maciej Banach, Martyna Fronczek, T. Osadnik, A. Gach, D. Strapagiel, M. Słomka, M. Lejawa, Anna Goc, E. Boniewska-Bernacka, Anna Pańczyszyn, G. Lip, P. Toth, P. Penson, J. Jóźwiak","doi":"10.5114/aoms/192147","DOIUrl":null,"url":null,"abstract":"Classical risk factors such as hypertension, hypercholesterolemia, pre-diabetes, diabetes and obesity can predict adverse cardiovascular events, but they are less prognostic in patients age <60 years. Polygenic risk scores (PRS) can be effective in predicting adverse coronary events in younger and middle-aged patients. Our main aim is to assess the utility of new PRS created for the Polish population in predicting mortality during an 8-year follow-up in a nationwide LIPIDOGEN2015 population.All DNA samples of 1779 patients were genotyped using Infinium Global Screening Array-24+ v3.0 Kit microarrays. The samples were amplified, fragmented, and hybridized to BeadChips. The BeadChips were scanned using iScan and converted to genotypes using Genome Studio 2.0.We will develop a PRS based on the marked single nucleotide polymorphisms (SNPs) in the LIPIDOGEN2015 project's studied population and determine the analyzed group's risk of death due to cardiovascular diseases (CVD) based on data obtained from 8-years of patient-follow-up. Based on the developed PRS scale and biochemical analyses, we will assess the effectiveness of lipid-lowering therapy with statins in patients with high and low genetic risk of sudden CVD events (secondary endpoints).The developed PRS scale, combined with clinical covariates, will facilitate the creation of an algorithm to predict long-term mortality. This will enable us to stratify CVD risk more precisely, which may result in earlier implementation of lifestyle changes and dietary adjustments and potentially initiate earlier pharmacotherapy for at-risk individuals.","PeriodicalId":8278,"journal":{"name":"Archives of Medical Science","volume":null,"pages":null},"PeriodicalIF":3.0000,"publicationDate":"2024-08-08","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Risk of adverse cardiovascular events based on common genetic variants in 8-year follow-up of the LIPIDOGEN2015 population using the polygenic risk score (PRS) - study design and methodology.\",\"authors\":\"Maciej Banach, Martyna Fronczek, T. Osadnik, A. Gach, D. Strapagiel, M. Słomka, M. Lejawa, Anna Goc, E. Boniewska-Bernacka, Anna Pańczyszyn, G. Lip, P. Toth, P. Penson, J. 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The BeadChips were scanned using iScan and converted to genotypes using Genome Studio 2.0.We will develop a PRS based on the marked single nucleotide polymorphisms (SNPs) in the LIPIDOGEN2015 project's studied population and determine the analyzed group's risk of death due to cardiovascular diseases (CVD) based on data obtained from 8-years of patient-follow-up. Based on the developed PRS scale and biochemical analyses, we will assess the effectiveness of lipid-lowering therapy with statins in patients with high and low genetic risk of sudden CVD events (secondary endpoints).The developed PRS scale, combined with clinical covariates, will facilitate the creation of an algorithm to predict long-term mortality. 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Risk of adverse cardiovascular events based on common genetic variants in 8-year follow-up of the LIPIDOGEN2015 population using the polygenic risk score (PRS) - study design and methodology.
Classical risk factors such as hypertension, hypercholesterolemia, pre-diabetes, diabetes and obesity can predict adverse cardiovascular events, but they are less prognostic in patients age <60 years. Polygenic risk scores (PRS) can be effective in predicting adverse coronary events in younger and middle-aged patients. Our main aim is to assess the utility of new PRS created for the Polish population in predicting mortality during an 8-year follow-up in a nationwide LIPIDOGEN2015 population.All DNA samples of 1779 patients were genotyped using Infinium Global Screening Array-24+ v3.0 Kit microarrays. The samples were amplified, fragmented, and hybridized to BeadChips. The BeadChips were scanned using iScan and converted to genotypes using Genome Studio 2.0.We will develop a PRS based on the marked single nucleotide polymorphisms (SNPs) in the LIPIDOGEN2015 project's studied population and determine the analyzed group's risk of death due to cardiovascular diseases (CVD) based on data obtained from 8-years of patient-follow-up. Based on the developed PRS scale and biochemical analyses, we will assess the effectiveness of lipid-lowering therapy with statins in patients with high and low genetic risk of sudden CVD events (secondary endpoints).The developed PRS scale, combined with clinical covariates, will facilitate the creation of an algorithm to predict long-term mortality. This will enable us to stratify CVD risk more precisely, which may result in earlier implementation of lifestyle changes and dietary adjustments and potentially initiate earlier pharmacotherapy for at-risk individuals.
期刊介绍:
Archives of Medical Science (AMS) publishes high quality original articles and reviews of recognized scientists that deal with all scientific medicine. AMS opens the possibilities for young, capable scientists. The journal would like to give them a chance to have a publication following matter-of-fact, professional review by outstanding, famous medical scientists. Thanks to that they will have an opportunity to present their study results and/or receive useful advice about the mistakes they have made so far.
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