Mitochondrial ATP synthase--a possible target protein in the regulation of energy metabolism in vitro and in vivo.

Berger, Karin; Sivars, Ulf; Sörhede Winzell, Maria; Johansson, Peter; Hellman, Ulf; Rippe, Catarina; Erlanson-Albertsson, Charlotte

Mitochondrial ATP synthase--a possible target protein in the regulation of energy metabolism in vitro and in vivo.

Mark

Berger, Karin ^LU

; Sivars, Ulf ; Sörhede Winzell, Maria ^LU ; Johansson, Peter ^LU ; Hellman, Ulf ; Rippe, Catarina ^LU and Erlanson-Albertsson, Charlotte ^LU (2002) In Nutritional Neuroscience 5(3). p.201-210

Abstract: The increasing prevalence of obesity in the Western world has stimulated an intense search for mechanisms regulating food intake and energy balance. A number of appetite-regulating peptides have been identified, their receptors cloned and the intracellular events characterized. One possible energy-dissipating mechanism is the mitochondrial uncoupling of ATP-synthesis from respiratory chain oxidation through uncoupling proteins, whereby energy derived from food could be dissipated as heat, instead of stored as ATP. The exact role of the uncoupling proteins in energy balance is, however, uncertain. We show here that mitochondrial F1F0-ATP synthase itself is a target protein for an anorectic peptide, enterostatin, demonstrated both after... (More); The increasing prevalence of obesity in the Western world has stimulated an intense search for mechanisms regulating food intake and energy balance. A number of appetite-regulating peptides have been identified, their receptors cloned and the intracellular events characterized. One possible energy-dissipating mechanism is the mitochondrial uncoupling of ATP-synthesis from respiratory chain oxidation through uncoupling proteins, whereby energy derived from food could be dissipated as heat, instead of stored as ATP. The exact role of the uncoupling proteins in energy balance is, however, uncertain. We show here that mitochondrial F1F0-ATP synthase itself is a target protein for an anorectic peptide, enterostatin, demonstrated both after affinity purification of rat brain membranes and through a direct physical interaction between enterostatin and purified F1-ATP synthase. In insulinoma cells (INS-1) enterostatin was found to target F1F0-ATP synthase, causing an inhibition of ATP production, an increased thermogenesis and increased oxygen consumption. The experiments suggest a role of mitochondrial F1F0-ATP synthase in the suppressed insulin secretion induced by enterostatin. It could be speculated that this targeting mechanism is involved in the decreased energy efficiency following enterostatin treatment in rat. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/108636

author

Berger, Karin ^LU

; Sivars, Ulf ; Sörhede Winzell, Maria ^LU ; Johansson, Peter ^LU ; Hellman, Ulf ; Rippe, Catarina ^LU and Erlanson-Albertsson, Charlotte ^LU

organization

publishing date

2002

type

Contribution to journal

publication status

published

subject

Basic Medicine

keywords

Ins-1, Enterostatin, Insulin, Thermogenesis, Uncoupling Protein

in

Nutritional Neuroscience

volume

5

issue

3

pages

201 - 210

publisher

Taylor & Francis

external identifiers

wos:000177387600004
pmid:12041876
scopus:0036014865

ISSN

1476-8305

DOI

10.1080/10284150290008604

language

English

LU publication?

yes

id

e0b6df51-dfb3-4364-bce3-d4d995346b20 (old id 108636)

date added to LUP

2016-04-01 12:10:48

date last changed

2024-01-08 11:16:49

@article{e0b6df51-dfb3-4364-bce3-d4d995346b20,
  abstract     = {{The increasing prevalence of obesity in the Western world has stimulated an intense search for mechanisms regulating food intake and energy balance. A number of appetite-regulating peptides have been identified, their receptors cloned and the intracellular events characterized. One possible energy-dissipating mechanism is the mitochondrial uncoupling of ATP-synthesis from respiratory chain oxidation through uncoupling proteins, whereby energy derived from food could be dissipated as heat, instead of stored as ATP. The exact role of the uncoupling proteins in energy balance is, however, uncertain. We show here that mitochondrial F1F0-ATP synthase itself is a target protein for an anorectic peptide, enterostatin, demonstrated both after affinity purification of rat brain membranes and through a direct physical interaction between enterostatin and purified F1-ATP synthase. In insulinoma cells (INS-1) enterostatin was found to target F1F0-ATP synthase, causing an inhibition of ATP production, an increased thermogenesis and increased oxygen consumption. The experiments suggest a role of mitochondrial F1F0-ATP synthase in the suppressed insulin secretion induced by enterostatin. It could be speculated that this targeting mechanism is involved in the decreased energy efficiency following enterostatin treatment in rat.}},
  author       = {{Berger, Karin and Sivars, Ulf and Sörhede Winzell, Maria and Johansson, Peter and Hellman, Ulf and Rippe, Catarina and Erlanson-Albertsson, Charlotte}},
  issn         = {{1476-8305}},
  keywords     = {{Ins-1; Enterostatin; Insulin; Thermogenesis; Uncoupling Protein}},
  language     = {{eng}},
  number       = {{3}},
  pages        = {{201--210}},
  publisher    = {{Taylor & Francis}},
  series       = {{Nutritional Neuroscience}},
  title        = {{Mitochondrial ATP synthase--a possible target protein in the regulation of energy metabolism in vitro and in vivo.}},
  url          = {{http://dx.doi.org/10.1080/10284150290008604}},
  doi          = {{10.1080/10284150290008604}},
  volume       = {{5}},
  year         = {{2002}},
}

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Mitochondrial ATP synthase--a possible target protein in the regulation of energy metabolism in vitro and in vivo.