Assembly and Secretion of VLDL in Nondifferentiated Caco-2 Cells Stably Transfected With Human Recombinant ApoB48 cDNA

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Arteriosclerosis, Thrombosis, and Vascular Biology. 1997;17:2955-2963

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Assembly and Secretion of VLDL in Nondifferentiated Caco-2 Cells Stably Transfected With Human Recombinant ApoB48 cDNA

Jayraz Luchoomun; Zhangyin Zhou; Ahmed Bakillah; Haris Jamil; ; M. Mahmood Hussain

From the Departments of Pathology (J.L., A.B., M.M.H.) and Biochemistry (Z.Z., M.M.H.), Allegheny University of the Health Sciences, MCP ${diamondsuit}$ Hahnemann School of Medicine, Philadelphia, Pa, and Bristol-Myers Squibb (H.J.), Pharmaceutical Research Institute, Princeton, NJ.

Correspondence to M. Mahmood Hussain, PhD, Allegheny University of the Health Sciences, MCP ${diamondsuit}$ Hahnemann School of Medicine, 2900 Queen Ln, Philadelphia, PA 19129. E-mail hussain{at}auhs.edu

Abstract Intestinal cells secrete apoB48-containing very low densitylipoproteins (VLDLs) and chylomicrons for the transport of biliaryand dietary lipids. The molecular mechanisms regulating the assemblyof intestinal lipoproteins are not known due to a lack of reliableand specific cell culture models. Caco-2 (a human colon carcinoma)cells have been used to study intestinal lipid metabolism. Thesecells have been shown to secrete both apoB100- and apoB48-containingtriglyceride (TG)-rich lipoproteins only after differentiationinto enterocyte-like cells. To study lipoprotein assembly innondifferentiated Caco-2 cells, we stably expressed human recombinantapoB48 cDNA under the control of a constitutive cytomegaloviruspromoter. Pulse-chase analysis revealed that the majority (>50%)of apoB48 synthesized was degraded intracellularly in the presenceor absence of oleic acid. Transfected nondifferentiated cellssecreted lipoproteins with flotation densities similar to thoseof plasma HDL or LDL when cultured in serum-free or serum-containingmedia, respectively. Incubation of cells with media containingserum and oleic acid resulted in the secretion of VLDL-like particles.Secretion of VLDL was inhibited (>80%) by triacsin C due to>60% inhibition of oleate-induced TG synthesis. However, inhibitionof cholesteryl ester synthesis by 70% with an acyl coenzyme A:cholesterolacyltransferase inhibitor did not affect VLDL secretion. Efficientassembly of lipoproteins usually requires the microsomal TGtransfer protein (MTP). The presence of MTP in transfected Caco-2cells was investigated by measuring TG transfer activity inmicrosomal fractions. Microsomal fractions had 0.2% TG transferactivity per hour per microgram of protein, which corresponds to30% to 60% of the MTP activity present in liver-derived cells. Todetermine whether MTP activity was required for lipoprotein assembly,transfected cells were incubated in the presence of the MTP inhibitorCP-10,447. This compound completely abolished the secretionof apoB. These data show that the transfected cell lines secretelipoproteins of different densities under different culture conditionsand that the assembly of larger VLDL particles requires activeTG synthesis and MTP activity. Thus, in nondifferentiated Caco-2 cells,the amount of apoB secreted and not the MTP activity is the limitingfactor for lipoprotein assembly.

Key Words: intestine • chylomicrons • triglycerides • apolipoprotein B • microsomal triglyceride transfer protein

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