Journal of Lipid Research (Dec 2018)

Genetic and secondary causes of severe HDL deficiency and cardiovascular disease1

  • Andrew S. Geller,
  • Eliana Y. Polisecki,
  • Margaret R. Diffenderfer,
  • Bela F. Asztalos,
  • Sotirios K. Karathanasis,
  • Robert A. Hegele,
  • Ernst J. Schaefer

Journal volume & issue
Vol. 59, no. 12
pp. 2421 – 2435

Abstract

Read online

We assessed secondary and genetic causes of severe HDL deficiency in 258,252 subjects, of whom 370 men (0.33%) and 144 women (0.099%) had HDL cholesterol levels G; 2) LCAT (12.4%): 1 homozygote, 3 compound heterozygotes, 13 heterozygotes, and 8 heterozygotes with variant rs4986970/p.S232T; 3) APOA1 (5.0%): 1 homozygote and 9 heterozygotes; and 4) LPL (4.5%): 1 heterozygote and 8 heterozygotes with variant rs268/p.N318S. In addition, 4.5% had other mutations, and 46.8% had no mutations. Atherosclerotic cardiovascular disease (ASCVD) prevalence rates in the ABCA1,LCAT,APOA1, LPL, and mutation-negative groups were 37.0%, 4.0%, 40.0%, 11.1%, and 6.4%, respectively. Severe HDL deficiency is uncommon, with 40.1% having secondary causes and 48.8% of the subjects sequenced having ABCA1,LCAT,APOA1, or LPL mutations or variants, with the highest ASCVD prevalence rates being observed in the ABCA1 and APOA1 groups.

Keywords