Journal of Lipid Research (Aug 2019)

ApoC-III ASO promotes tissue LPL activity in the absence of apoE-mediated TRL clearance

  • Bastian Ramms,
  • Sohan Patel,
  • Chelsea Nora,
  • Ariane R. Pessentheiner,
  • Max W. Chang,
  • Courtney R. Green,
  • Gregory J. Golden,
  • Patrick Secrest,
  • Ronald M. Krauss,
  • Christian M. Metallo,
  • Christopher Benner,
  • Veronica J. Alexander,
  • Joseph L. Witztum,
  • Sotirios Tsimikas,
  • Jeffrey D. Esko,
  • Philip L.S.M. Gordts

Journal volume & issue
Vol. 60, no. 8
pp. 1379 – 1395

Abstract

Read online

Hypertriglyceridemia results from accumulation of triglyceride (TG)-rich lipoproteins (TRLs) in the circulation and is associated with increased CVD risk. ApoC-III is an apolipoprotein on TRLs and a prominent negative regulator of TG catabolism. We recently established that in vivo apoC-III predominantly inhibits LDL receptor-mediated and LDL receptor-related protein 1-mediated hepatic TRL clearance and that apoC-III-enriched TRLs are preferentially cleared by syndecan-1 (SDC1). In this study, we determined the impact of apoE, a common ligand for all three receptors, on apoC-III metabolism using apoC-III antisense oligonucleotide (ASO) treatment in mice lacking apoE and functional SDC1 (Apoe−/−Ndst1f/fAlb-Cre+). ApoC-III ASO treatment significantly reduced plasma TG levels in Apoe−/−Ndst1f/fAlb-Cre+ mice without reducing hepatic VLDL production or improving hepatic TRL clearance. Further analysis revealed that apoC-III ASO treatment lowered plasma TGs in Apoe−/−Ndst1f/fAlb-Cre+ mice, which was associated with increased LPL activity in white adipose tissue in the fed state. Finally, clinical data confirmed that ASO-mediated lowering of APOC-III via volanesorsen can reduce plasma TG levels independent of the APOE isoform genotype. Our data indicate that apoE determines the metabolic impact of apoC-III as we establish that apoE is essential to mediate inhibition of TRL clearance by apoC-III and that, in the absence of functional apoE, apoC-III inhibits tissue LPL activity.

Keywords