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Pharmacogenetic loci for rosuvastatin are associated with intima-media thickness change and coronary artery disease risk

  • Published:2022-01 Issue:1 Volume:23 Page:15-34
  • ISSN:1462-2416
  • Container-title:Pharmacogenomics
  • language:en
  • Short-container-title:Pharmacogenomics

Author:

Kononov Stanislav1ORCID,Mal Galina2ORCID,Azarova Iuliia34ORCID,Klyosova Elena45ORCID,Bykanova Marina56ORCID,Churnosov Mikhail7ORCID,Polonikov Alexey58ORCID

Affiliation:

1. Department of Internal Medicine N 2, Kursk State Medical University, 14 Pirogova St., Kursk 305035, Russian Federation

2. Department of Pharmacology, Kursk State Medical University, 3 Karl Marx St., Kursk 305041, Russian Federation

3. Department of Biological Chemistry, Kursk State Medical University, 3 Karl Marx St., Kursk 305041, Russian Federation

4. Laboratory of Biochemical Genetics & Metabolomics, Research Institute for Genetic & Molecular Epidemiology, Kursk State Medical University, 18 Yamskaya St., Kursk 305041, Russian Federation

5. Department of Biology, Medical Genetics & Ecology, Kursk State Medical University, 3 Karl Marx St., Kursk 305041, Russian Federation

6. Laboratory of Genomic Research, Research Institute for Genetic & Molecular Epidemiology, Kursk State Medical University, 18 Yamskaya St., Kursk 305041, Russian Federation

7. Department of Medical Biological Disciplines, Belgorod State University, 85 Pobeda St., Belgorod 308015, Russian Federation

8. Laboratory of Statistical Genetics & Bioinformatics, Research Institute for Genetic & Molecular Epidemiology, Kursk State Medical University, 18 Yamskaya St., Kursk 305041, Russian Federation

Abstract

Aim: Polymorphisms at LPA, LDLR, APOE, APOC1, MYLIP and ABCG2 are attractive targets for assessment of their impact on lipid-lowering therapy with rosuvastatin. The present study investigated whether polymorphisms at these genes are associated with the risk of coronary artery disease (CAD) development, and reduction of atherogenic lipids and carotid intima-media thickness (CIMT) in CAD patients, taking rosuvastatin. Materials & methods: 190 CAD patients and 1697 subjects were enrolled in pharmacogenetic and genetic association study, respectively. SNP genotyping was done using the MassARRAY-4 system. Results: MYLIP rs6924995, rs3757354, APOC1 rs445925, LDLR rs6511720, APOE rs7412, ABCG2 rs2199936, rs1481012 variants were significantly associated with CAD susceptibility (p = 0.016, 0.0003, <0.0001, <0.0001, 0.013, 0.016, 0.0035, respectively), as well as with CIMT regression (except ABCG2 variants; p = 0.05, 0.039, 0.039, 0.016, 0.0065), and changes in plasma lipids during rosuvastatin therapy. Conclusion: The studied polymorphisms possess pleiotropic effects on plasma lipids and CIMT, CAD susceptibility, and determine lipid-lowering response to rosuvastatin.

Publisher

Future Medicine Ltd

Subject

Pharmacology,Genetics,Molecular Medicine
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