Accelerated lipoprotein uptake by transplantable hepatomas that express hepatic lipase

To test the hypothesis that hepatic lipase plays a key role in lipoprotein removal in vivo, a novel system was used. Hepatoma cells (HTC 7288c) were transfected with a cDNA encoding hepatic lipase in culture and grown as solid tumors in vivo. In culture, transfected cells degraded chylomicron remnan...

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Main Authors: Charles Donner, Sungshin Choi, Michael Komaromy, Allen D. Cooper
Format: Article
Language:English
Published: Elsevier 1998-09-01
Series:Journal of Lipid Research
Subjects:
LDL
Online Access:http://www.sciencedirect.com/science/article/pii/S0022227520321684
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spelling doaj-61dca8f665264a9c90875e25831b233f2021-04-26T13:50:00ZengElsevierJournal of Lipid Research0022-22751998-09-0139918051815Accelerated lipoprotein uptake by transplantable hepatomas that express hepatic lipaseCharles Donner0Sungshin Choi1Michael Komaromy2Allen D. Cooper3Research Institute, Palo Alto Medical Foundation, 860 Bryant St., Palo Alto, CA 94301; Department of Medicine, Stanford University School of Medicine, Stanford, CA 94305Research Institute, Palo Alto Medical Foundation, 860 Bryant St., Palo Alto, CA 94301Research Institute, Palo Alto Medical Foundation, 860 Bryant St., Palo Alto, CA 94301To whom correspondence should be addressed.; Research Institute, Palo Alto Medical Foundation, 860 Bryant St., Palo Alto, CA 94301; Department of Medicine, Stanford University School of Medicine, Stanford, CA 94305To test the hypothesis that hepatic lipase plays a key role in lipoprotein removal in vivo, a novel system was used. Hepatoma cells (HTC 7288c) were transfected with a cDNA encoding hepatic lipase in culture and grown as solid tumors in vivo. In culture, transfected cells degraded chylomicron remnants and low density lipoprotein (LDL) somewhat more efficiently than untransfected cells. Tumors from the transplanted cells produced hepatic lipase localized to the surface of tumors from transfected cells but not tumors from non-transfected cells, grown in the same rat. The tumors from transfected cells removed, per gm of tissue, 34% (P < 0.001) more 125I-labeled LDL than tumors from non-transfected cells in the same animal. The uptake of chylomicron remnants (by tumors from transfected cells) was also modestly enhanced (15 ± 6%, P < 0.005). There were no differences in the uptake of 125I-labeled albumin or 125I-labeled asialoglycoprotein. Compared to the liver, the untransfected tumors took up 12%, and the transfected tumors took up about 18% as much LDL per gram of tissue. The uptake of chylomicron remnants compared to liver was far lower. Both types of tumors had about twice as much LDL receptor related protein as the liver. Wild-type tumors had the highest level of LDL receptor, twice hepatic lipase-secreting tumors, and six times that of the liver. Using the novel approach of transfecting transplantable tumor cells with hepatic lipase, the ability of hepatic lipase to facilitate the removal of apoB-containing lipoproteins was demonstrated. The liver still removes low density lipoprotein and especially chylomicron remnants more rapidly than the tumors, suggesting factors in addition to hepatic lipase and LDL receptor level play a major role in hepatic lipoprotein removal.—Donner, C., S. Choi, M. Komaromy, and A. D. Cooper. Accelerated lipoprotein uptake by transplantable hepatomas that express hepatic lipase.http://www.sciencedirect.com/science/article/pii/S0022227520321684hepatic lipaseLDLchylomicron remnantlipoprotein lipase
collection DOAJ
language English
format Article
sources DOAJ
author Charles Donner
Sungshin Choi
Michael Komaromy
Allen D. Cooper
spellingShingle Charles Donner
Sungshin Choi
Michael Komaromy
Allen D. Cooper
Accelerated lipoprotein uptake by transplantable hepatomas that express hepatic lipase
Journal of Lipid Research
hepatic lipase
LDL
chylomicron remnant
lipoprotein lipase
author_facet Charles Donner
Sungshin Choi
Michael Komaromy
Allen D. Cooper
author_sort Charles Donner
title Accelerated lipoprotein uptake by transplantable hepatomas that express hepatic lipase
title_short Accelerated lipoprotein uptake by transplantable hepatomas that express hepatic lipase
title_full Accelerated lipoprotein uptake by transplantable hepatomas that express hepatic lipase
title_fullStr Accelerated lipoprotein uptake by transplantable hepatomas that express hepatic lipase
title_full_unstemmed Accelerated lipoprotein uptake by transplantable hepatomas that express hepatic lipase
title_sort accelerated lipoprotein uptake by transplantable hepatomas that express hepatic lipase
publisher Elsevier
series Journal of Lipid Research
issn 0022-2275
publishDate 1998-09-01
description To test the hypothesis that hepatic lipase plays a key role in lipoprotein removal in vivo, a novel system was used. Hepatoma cells (HTC 7288c) were transfected with a cDNA encoding hepatic lipase in culture and grown as solid tumors in vivo. In culture, transfected cells degraded chylomicron remnants and low density lipoprotein (LDL) somewhat more efficiently than untransfected cells. Tumors from the transplanted cells produced hepatic lipase localized to the surface of tumors from transfected cells but not tumors from non-transfected cells, grown in the same rat. The tumors from transfected cells removed, per gm of tissue, 34% (P < 0.001) more 125I-labeled LDL than tumors from non-transfected cells in the same animal. The uptake of chylomicron remnants (by tumors from transfected cells) was also modestly enhanced (15 ± 6%, P < 0.005). There were no differences in the uptake of 125I-labeled albumin or 125I-labeled asialoglycoprotein. Compared to the liver, the untransfected tumors took up 12%, and the transfected tumors took up about 18% as much LDL per gram of tissue. The uptake of chylomicron remnants compared to liver was far lower. Both types of tumors had about twice as much LDL receptor related protein as the liver. Wild-type tumors had the highest level of LDL receptor, twice hepatic lipase-secreting tumors, and six times that of the liver. Using the novel approach of transfecting transplantable tumor cells with hepatic lipase, the ability of hepatic lipase to facilitate the removal of apoB-containing lipoproteins was demonstrated. The liver still removes low density lipoprotein and especially chylomicron remnants more rapidly than the tumors, suggesting factors in addition to hepatic lipase and LDL receptor level play a major role in hepatic lipoprotein removal.—Donner, C., S. Choi, M. Komaromy, and A. D. Cooper. Accelerated lipoprotein uptake by transplantable hepatomas that express hepatic lipase.
topic hepatic lipase
LDL
chylomicron remnant
lipoprotein lipase
url http://www.sciencedirect.com/science/article/pii/S0022227520321684
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