Insulin stimulates the uptake of chylomicron remnants in cultured rat hepatocytes

Jensen, Elmo; Florén, Claes-Henrik; Nilsson, Åke

Insulin stimulates the uptake of chylomicron remnants in cultured rat hepatocytes

Mark

Jensen, Elmo ; Florén, Claes-Henrik ^LU and Nilsson, Åke ^LU (1988) In European Journal of Clinical Investigation 18(3). p.226-232

Abstract: The effects of insulin (10-1000 microU ml-1) on chylomicron remnant uptake and degradation were studied in hepatocyte monolayer cultures. Both uptake and degradation were stimulated by insulin. The degree of stimulation was influenced by cell density, being most pronounced in sparse cultures. The uptake was stimulated in a dose-dependent fashion and was noticed already at a physiological insulin level (100 microU ml-1). At this insulin concentration uptake was stimulated by approximately 50% (range 26-84%). As suggested by the increase in Vmax for the remnant uptake, the number of lipoprotein receptors on the hepatocytes was increased by 100 microU ml-1 of insulin. Apolipoprotein-E-free low density lipoproteins (LDL) competed much less... (More); The effects of insulin (10-1000 microU ml-1) on chylomicron remnant uptake and degradation were studied in hepatocyte monolayer cultures. Both uptake and degradation were stimulated by insulin. The degree of stimulation was influenced by cell density, being most pronounced in sparse cultures. The uptake was stimulated in a dose-dependent fashion and was noticed already at a physiological insulin level (100 microU ml-1). At this insulin concentration uptake was stimulated by approximately 50% (range 26-84%). As suggested by the increase in Vmax for the remnant uptake, the number of lipoprotein receptors on the hepatocytes was increased by 100 microU ml-1 of insulin. Apolipoprotein-E-free low density lipoproteins (LDL) competed much less efficiently for the uptake of radioactive remnants than did unlabelled remnant particles. About half of the stimulatory effect of insulin on the remnant uptake could, however, be abolished by adding an excess of LDL, indicating that at least part of the stimulation by insulin was due to increased activity of the LDL receptor. This study thus shows that physiological insulin levels increase chylomicron remnant uptake in hepatocyte monolayer cultures. It is assumed that the effect of insulin is to increase the number of lipoprotein receptors at the cell surface, and at least part of the stimulation is due to an increase in LDL receptor (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/14169da1-3e67-46ec-a691-4d618f6d3dd1

author

Jensen, Elmo ; Florén, Claes-Henrik ^LU and Nilsson, Åke ^LU

publishing date

1988-06-01

type

Contribution to journal

publication status

published

in

European Journal of Clinical Investigation

volume

18

issue

3

pages

7 pages

publisher

Wiley-Blackwell

external identifiers

scopus:0023948572

ISSN

0014-2972

language

English

LU publication?

no

id

14169da1-3e67-46ec-a691-4d618f6d3dd1

date added to LUP

2019-05-30 16:54:39

date last changed

2021-03-23 22:00:40

@article{14169da1-3e67-46ec-a691-4d618f6d3dd1,
  abstract     = {{The effects of insulin (10-1000 microU ml-1) on chylomicron remnant uptake and degradation were studied in hepatocyte monolayer cultures. Both uptake and degradation were stimulated by insulin. The degree of stimulation was influenced by cell density, being most pronounced in sparse cultures. The uptake was stimulated in a dose-dependent fashion and was noticed already at a physiological insulin level (100 microU ml-1). At this insulin concentration uptake was stimulated by approximately 50% (range 26-84%). As suggested by the increase in Vmax for the remnant uptake, the number of lipoprotein receptors on the hepatocytes was increased by 100 microU ml-1 of insulin. Apolipoprotein-E-free low density lipoproteins (LDL) competed much less efficiently for the uptake of radioactive remnants than did unlabelled remnant particles. About half of the stimulatory effect of insulin on the remnant uptake could, however, be abolished by adding an excess of LDL, indicating that at least part of the stimulation by insulin was due to increased activity of the LDL receptor. This study thus shows that physiological insulin levels increase chylomicron remnant uptake in hepatocyte monolayer cultures. It is assumed that the effect of insulin is to increase the number of lipoprotein receptors at the cell surface, and at least part of the stimulation is due to an increase in LDL receptor}},
  author       = {{Jensen, Elmo and Florén, Claes-Henrik and Nilsson, Åke}},
  issn         = {{0014-2972}},
  language     = {{eng}},
  month        = {{06}},
  number       = {{3}},
  pages        = {{226--232}},
  publisher    = {{Wiley-Blackwell}},
  series       = {{European Journal of Clinical Investigation}},
  title        = {{Insulin stimulates the uptake of chylomicron remnants in cultured rat hepatocytes}},
  volume       = {{18}},
  year         = {{1988}},
}

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Insulin stimulates the uptake of chylomicron remnants in cultured rat hepatocytes