Plasminogen promotes cholesterol efflux by the ABCA1 pathway
Nathalie Pamir, Patrick M. Hutchins, Graziella E. Ronsein, Hao Wei, Chongren Tang, Riku Das, Tomas Vaisar, Edward Plow, Volker Schuster, Marlys L. Koschinsky, Catherine A. Reardon, Richard Weinberg, David A. Dichek, Santica Marcovina, Godfrey S. Getz, Jay W. Heinecke
Nathalie Pamir, Patrick M. Hutchins, Graziella E. Ronsein, Hao Wei, Chongren Tang, Riku Das, Tomas Vaisar, Edward Plow, Volker Schuster, Marlys L. Koschinsky, Catherine A. Reardon, Richard Weinberg, David A. Dichek, Santica Marcovina, Godfrey S. Getz, Jay W. Heinecke
View: Text | PDF
Research Article Endocrinology Metabolism

Plasminogen promotes cholesterol efflux by the ABCA1 pathway

Abstract

Using genetic and biochemical approaches, we investigated proteins that regulate macrophage cholesterol efflux capacity (CEC) and ABCA1-specific CEC (ABCA1 CEC), 2 functional assays that predict cardiovascular disease (CVD). Macrophage CEC and the concentration of HDL particles were markedly reduced in mice deficient in apolipoprotein A-I (APOA1) or apolipoprotein E (APOE) but not apolipoprotein A-IV (APOA4). ABCA1 CEC was markedly reduced in APOA1-deficient mice but was barely affected in mice deficient in APOE or APOA4. High-resolution size-exclusion chromatography of plasma produced 2 major peaks of ABCA1 CEC activity. The early-eluting peak, which coeluted with HDL, was markedly reduced in APOA1- or APOE-deficient mice. The late-eluting peak was modestly reduced in APOA1-deficient mice but little affected in APOE- or APOA4-deficient mice. Ion-exchange chromatography and shotgun proteomics suggested that plasminogen (PLG) accounted for a substantial fraction of the ABCA1 CEC activity in the peak not associated with HDL. Human PLG promoted cholesterol efflux by the ABCA1 pathway, and PLG-dependent efflux was inhibited by lipoprotein(a) [Lp(a)]. Our observations identify APOA1, APOE, and PLG as key determinants of CEC. Because PLG and Lp(a) associate with human CVD risk, interplay among the proteins might affect atherosclerosis by regulating cholesterol efflux from macrophages.

Authors

Nathalie Pamir, Patrick M. Hutchins, Graziella E. Ronsein, Hao Wei, Chongren Tang, Riku Das, Tomas Vaisar, Edward Plow, Volker Schuster, Marlys L. Koschinsky, Catherine A. Reardon, Richard Weinberg, David A. Dichek, Santica Marcovina, Godfrey S. Getz, Jay W. Heinecke

×

Figure 1

Macrophage cholesterol efflux capacity (CEC) and ABCA1-specific CEC (ABCA1 CEC) for wild-type mice and mice deficient in APOA1, APOE, APOA1/APOE, or APOA4.

Options: View larger image (or click on image) Download as PowerPoint
Macrophage cholesterol efflux capacity (CEC) and ABCA1-specific CEC (ABC...
Serum HDL (APOB-depleted serum) was obtained by polyethylene glycol precipitation of plasma-derived serum of wild-type mice (WT, n = 6), Apoa1–/– mice (n = 6), Apoe–/– mice (n = 6), Apoa1–/–; Apoe–/– mice (n = 3), or Apoa4–/– mice (n = 3). (A) Macrophage CEC and (B) ABCA1 CEC of serum HDL were monitored using [3H]cholesterol-labeled J774 macrophages and baby hamster kidney (BHK) cells, respectively. Cholesterol efflux was calculated as the percentage of radiolabel in the medium of the cells at the end of a 4-hour incubation divided by the total radioactivity of the medium and cells. Macrophage CEC and ABCA1 CEC were quantified as the difference in cholesterol efflux of cells with and without exposure to cAMP and with or without induction of ABCA1 expression, respectively. Significance was determined by ANOVA followed by a Fisher’s post-hoc analysis for multiple comparisons. *P < 0.05 versus wild-type mice.