Metabolomic Consequences of Genetic Inhibition of PCSK9 Compared With Statin Treatment

Eeva Sliz(Biocenter Finland), Johannes Kettunen(Biocenter Finland), Michael V. Holmes(National Institute for Health and Care Research), Clare Oliver Williams(University of Cambridge), Charles Boachie(The Robertson Trust), Qin Wang(Baker Heart and Diabetes Institute), Minna Männikkö(University of Oulu), Sylvain Sebért(Biocenter Finland), Robin Walters(Nuffield Health), Kuang Lin(Nuffield Health), Iona Y. Millwood(Nuffield Health), Robert B. Clarke(Nuffield Health), Liming Li(Chinese Academy of Medical Sciences & Peking Union Medical College), Naomi Rankin(University of Glasgow), Paul Welsh(The Welding Institute), Christian Delles(Nippon Sheet Glass (United Kingdom)), J. Wouter Jukema(Leiden University Medical Center), Stella Trompet(Leiden University Medical Center), Ian Ford(The Robertson Trust), Markus Perola(Estonian University of Life Sciences), Veikko Salomaa(Finnish Institute for Health and Welfare), Marjo‐Riitta Järvelin(Oulu University Hospital), Zhengming Chen(Nuffield Health), Debbie A. Lawlor(University of Bristol), Mika Ala‐Korpela(University of Bristol), John Danesh(Wellcome Sanger Institute), George Davey Smith(University of Bristol), Naveed Sattar(University of Glasgow), Adam S. Butterworth(National Institute for Health and Care Research), Peter Würtz(University of Helsinki)
Circulation
November 27, 2018
10.1161/circulationaha.118.034942
Cited by 117Open Access
Full Text

Abstract

Background: Both statins and proprotein convertase subtilisin/kexin type 9 (PCSK9) inhibitors lower blood low-density lipoprotein cholesterol levels to reduce risk of cardiovascular events. To assess potential differences between metabolic effects of these 2 lipid-lowering therapies, we performed detailed lipid and metabolite profiling of a large randomized statin trial and compared the results with the effects of genetic inhibition of PCSK9, acting as a naturally occurring trial. Methods: Two hundred twenty-eight circulating metabolic measures were quantified by nuclear magnetic resonance spectroscopy, including lipoprotein subclass concentrations and their lipid composition, fatty acids, and amino acids, for 5359 individuals (2659 on treatment) in the PROSPER (Prospective Study of Pravastatin in the Elderly at Risk) trial at 6 months postrandomization. The corresponding metabolic measures were analyzed in 8 population cohorts (N=72 185) using PCSK9 rs11591147 as an unconfounded proxy to mimic the therapeutic effects of PCSK9 inhibitors. Results: Scaled to an equivalent lowering of low-density lipoprotein cholesterol, the effects of genetic inhibition of PCSK9 on 228 metabolic markers were generally consistent with those of statin therapy ( R 2 =0.88). Alterations in lipoprotein lipid composition and fatty acid distribution were similar. However, discrepancies were observed for very-low-density lipoprotein lipid measures. For instance, genetic inhibition of PCSK9 had weaker effects on lowering of very-low-density lipoprotein cholesterol compared with statin therapy (54% versus 77% reduction, relative to the lowering effect on low-density lipoprotein cholesterol; P =2×10 -7 for heterogeneity). Genetic inhibition of PCSK9 showed no significant effects on amino acids, ketones, or a marker of inflammation (GlycA), whereas statin treatment weakly lowered GlycA levels. Conclusions: Genetic inhibition of PCSK9 had similar metabolic effects to statin therapy on detailed lipid and metabolite profiles. However, PCSK9 inhibitors are predicted to have weaker effects on very-low-density lipoprotein lipids compared with statins for an equivalent lowering of low-density lipoprotein cholesterol, which potentially translate into smaller reductions in cardiovascular disease risk.

Related Papers

No related papers found

Powered by citation graph analysis