Mathematical modelling of competitive LDL/VLDL binding and uptake by hepatocytes

Elevated levels of low-density-lipoprotein cholesterol (LDL-C) in the plasma are a well-established risk factor for the development of coronary heart disease. Plasma LDL-C levels are in part determined by the rate at which LDL particles are removed from the bloodstream by hepatic uptake. The uptake of LDL by mammalian liver cells occurs mainly via receptor-mediated endocytosis, a process which entails the binding of these particles to specific receptors in specialised areas of the cell surface, the subsequent internalization of the receptor–lipoprotein complex, and ultimately the degradation and release of the ingested lipoproteins’ constituent parts. We formulate a mathematical model to study the binding and internalization (endocytosis) of LDL and VLDL particles by hepatocytes in culture. The system of ordinary differential equations, which includes a cholesterol-dependent pit production term representing feedback regulation of surface receptors in response to intracellular cholesterol levels, is analysed using numerical simulations and steady-state analysis. Our numerical results show good agreement with in vitro experimental data describing LDL uptake by cultured hepatocytes following delivery of a single bolus of lipoprotein. Our model is adapted in order to reflect the in vivo situation, in which lipoproteins are continuously delivered to the hepatocyte. In this case, our model suggests that the competition between the LDL and VLDL particles for binding to the pits on the cell surface affects the intracellular cholesterol concentration. In particular, we predict that when there is continuous delivery of low levels of lipoproteins to the cell surface, more VLDL than LDL occupies the pit, since VLDL are better competitors for receptor binding. VLDL have a cholesterol content comparable to LDL particles; however, due to the larger size of VLDL, one pit-bound VLDL particle blocks binding of several LDLs, and there is a resultant drop in the intracellular cholesterol level. When there is continuous delivery of lipoprotein at high levels to the hepatocytes, VLDL particles still out-compete LDL particles for receptor binding, and consequently more VLDL than LDL particles occupy the pit. Although the maximum intracellular cholesterol level is similar for high and low levels of lipoprotein delivery, the maximum is reached more rapidly when the lipoprotein delivery rates are high. The implications of these results for the design of in vitro experiments is discussed.

[1]  G. Watts,et al.  Apolipoprotein B-100 kinetics in visceral obesity: associations with plasma apolipoprotein C-III concentration. , 2002, Metabolism: clinical and experimental.

[2]  Joseph L. Goldstein,et al.  Coated pits, coated vesicles, and receptor-mediated endocytosis , 1979, Nature.

[3]  F. Maxfield,et al.  Iterative fractionation of recycling receptors from lysosomally destined ligands in an early sorting endosome , 1989, The Journal of cell biology.

[4]  H. J. Harwood,et al.  Kinetics of low-density lipoprotein receptor activity in Hep-G2 cells: derivation and validation of a Briggs-Haldane-based kinetic model for evaluating receptor-mediated endocytotic processes in which receptors recycle. , 1997, The Biochemical journal.

[5]  L. Havekes,et al.  Cellular free cholesterol in Hep G2 cells is only partially available for down-regulation of low-density-lipoprotein receptor activity. , 1987, The Biochemical journal.

[6]  E. Johnson,et al.  Contribution of apoB-48 and apoB-100 triglyceride-rich lipoproteins (TRL) to postprandial increases in the plasma concentration of TRL triglycerides and retinyl esters. , 1993, Journal of lipid research.

[7]  J. Herz,et al.  Role of the low density lipoprotein receptor in the flux of cholesterol through the plasma and across the tissues of the mouse. , 1995, The Journal of clinical investigation.

[8]  K. Parker,et al.  A Dynamical Model of Lipoprotein Metabolism , 2006, Bulletin of mathematical biology.

[9]  M. Brown,et al.  Receptor-mediated endocytosis: insights from the lipoprotein receptor system. , 1979, Proceedings of the National Academy of Sciences of the United States of America.

[10]  M. Brown,et al.  Characterization of the low density lipoprotein receptor in membranes prepared from human fibroblasts. , 1978, The Journal of biological chemistry.

[11]  A. Häkkinen,et al.  Overproduction of large VLDL particles is driven by increased liver fat content in man , 2006, Diabetologia.

[12]  H. M. Byrne,et al.  Mathematical Model for Low Density Lipoprotein (LDL) Endocytosis by Hepatocytes , 2008, Bulletin of mathematical biology.

[13]  Christine M. Williams,et al.  Saturated fat-induced changes in Sf 60–400 particle composition reduces uptake of LDL by HepG2 cells Published, JLR Papers in Press, November 8, 2005. , 2006, Journal of Lipid Research.

[14]  J Panovska-Griffiths,et al.  Mathematical models of hepatic lipoprotein , 2005 .