ApoC-III inhibits clearance of triglyceride-rich lipoproteins through LDL family receptors
Philip L.S.M. Gordts, … , Joseph L. Witztum, Jeffrey D. Esko
Philip L.S.M. Gordts, … , Joseph L. Witztum, Jeffrey D. Esko
Published July 11, 2016
Citation Information: J Clin Invest. 2016;126(8):2855-2866. https://doi.org/10.1172/JCI86610.
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Research Article Metabolism

ApoC-III inhibits clearance of triglyceride-rich lipoproteins through LDL family receptors

Abstract

Hypertriglyceridemia is an independent risk factor for cardiovascular disease, and plasma triglycerides (TGs) correlate strongly with plasma apolipoprotein C-III (ApoC-III) levels. Antisense oligonucleotides (ASOs) for ApoC-III reduce plasma TGs in primates and mice, but the underlying mechanism of action remains controversial. We determined that a murine-specific ApoC-III–targeting ASO reduces fasting TG levels through a mechanism that is dependent on low-density lipoprotein receptors (LDLRs) and LDLR-related protein 1 (LRP1). ApoC-III ASO treatment lowered plasma TGs in mice lacking lipoprotein lipase (LPL), hepatic heparan sulfate proteoglycan (HSPG) receptors, LDLR, or LRP1 and in animals with combined deletion of the genes encoding HSPG receptors and LDLRs or LRP1. However, the ApoC-III ASO did not lower TG levels in mice lacking both LDLR and LRP1. LDLR and LRP1 were also required for ApoC-III ASO–induced reduction of plasma TGs in mice fed a high-fat diet, in postprandial clearance studies, and when ApoC-III–rich or ApoC-III–depleted lipoproteins were injected into mice. ASO reduction of ApoC-III had no effect on VLDL secretion, heparin-induced TG reduction, or uptake of lipids into heart and skeletal muscle. Our data indicate that ApoC-III inhibits turnover of TG-rich lipoproteins primarily through a hepatic clearance mechanism mediated by the LDLR/LRP1 axis.

Authors

Philip L.S.M. Gordts, Ryan Nock, Ni-Huiping Son, Bastian Ramms, Irene Lew, Jon C. Gonzales, Bryan E. Thacker, Debapriya Basu, Richard G. Lee, Adam E. Mullick, Mark J. Graham, Ira J. Goldberg, Rosanne M. Crooke, Joseph L. Witztum, Jeffrey D. Esko

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Figure 7

ApoC-III ASO treatment does not alter in vivo LPL activity or VLDL production.

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ApoC-III ASO treatment does not alter in vivo LPL activity or VLDL produ...
(A and B) Plasma TGs were measured before and after heparin injection in WT, Ldlr–/– Ndst1fl/fl Alb-Cre+, and Ldlr–/– Lrp1fl/fl Alb-Cre+ mice treated for 4 weeks with control or ApoC-III ASO (A) after an overnight fast or (B) 3 hours after a fat challenge. Heparin was injected i.v. (50 U/mouse), and blood was sampled via tail-vein bleeding 10 minutes after injection (n = 3–5/group). (C) Hepatic VLDL production was determined in overnight-fasted Ldlr–/– Lrp1fl/fl Alb-Cre+ mice after injection with tyloxapol to inhibit lipolysis. Blood samples were collected at the indicated time points and processed to measure plasma TG accumulation and VLDL production rates (n = 3/group). Values represent the mean ± SEM. ANOVA with Bonferroni’s post-hoc test.