Fasting reveals largely intact systemic lipid mobilization mechanisms in respiratory chain complex III deficient mice.

Tomasic, Nikica; Kotarsky, Heike; de Oliveira Figueiredo, Rejane; Hansson, Eva; Mörgelin, Matthias; Tomasic, Ivan; Kallijärvi, Jukka; Elmér, Eskil; Jauhiainen, Matti; Eklund, Erik A; Fellman, Vineta

Tomasic, Nikica; Kotarsky, Heike; de Oliveira Figueiredo, Rejane; Hansson, Eva; Mörgelin, Matthias; Tomasic, Ivan; Kallijärvi, Jukka; Elmér, Eskil; Jauhiainen, Matti; Eklund, Erik A; Fellman, Vineta.

Afiliación

Tomasic N; Lund University, Department of Clinical Sciences, Lund, Pediatrics, Lund, Sweden; Karolinska University Hospital, Department of Neonatology, Stockholm, Sweden; Faculty of Science, Department of Biology, University of Zagreb, Croatia. Electronic address: nikica.tomasic@med.lu.se.
Kotarsky H; Department of Pathology, Region Skåne, Lund University, Sweden.
de Oliveira Figueiredo R; Folkhälsan Research Center, Helsinki, Finland. Electronic address: rejane.figueiredo@helsinki.fi.
Hansson E; Lund University, Department of Clinical Sciences, Lund, Pediatrics, Lund, Sweden. Electronic address: eva.hansson@med.lu.se.
Mörgelin M; Lund University, Department of Clinical Sciences, Lund, Lund, Sweden. Electronic address: matthias@colzyx.com.
Tomasic I; Mälardalen University, Division of Intelligent Future Technologies, Västerås, Sweden. Electronic address: ivan.tomasic@mdh.se.
Kallijärvi J; Folkhälsan Research Center, Helsinki, Finland; Stem Cells and Metabolism Research Program, Faculty of Medicine, University of Helsinki, Helsinki, Finland. Electronic address: jukka.kallijarvi@helsinki.fi.
Elmér E; Department of Clinical Sciences, Lund, Mitochondrial Medicine, Lund University, Lund, Sweden. Electronic address: eskil.elmer@med.lu.se.
Jauhiainen M; Minerva Foundation Institute for Medical Research, Biomedicum 2U, National Institute for Health and Welfare, Helsinki, Finland. Electronic address: matti.jauhiainen@thl.fi.
Eklund EA; Lund University, Department of Clinical Sciences, Lund, Pediatrics, Lund, Sweden. Electronic address: erik.eklund@med.lu.se.
Fellman V; Lund University, Department of Clinical Sciences, Lund, Pediatrics, Lund, Sweden; Folkhälsan Research Center, Helsinki, Finland; Children's Hospital, University of Helsinki, Helsinki. Finland. Electronic address: vineta.fellman@med.lu.se.

Biochim Biophys Acta Mol Basis Dis ; 1866(1): 165573, 2020 01 01.

Article en En | MEDLINE | ID: mdl-31672551

ABSTRACT

ABSTRACT

Mice homozygous for the human GRACILE syndrome mutation (Bcs1lc.A232G) display decreased respiratory chain complex III activity, liver dysfunction, hypoglycemia, rapid loss of white adipose tissue and early death. To assess the underlying mechanism of the lipodystrophy in homozygous mice (Bcs1lp.S78G), these and wild-type control mice were subjected to a short 4-hour fast. The homozygotes had low baseline blood glucose values, but a similar decrease in response to fasting as in wild-type mice, resulting in hypoglycemia in the majority. Despite the already depleted glycogen and increased triacylglycerol content in the mutant livers, the mice responded to fasting by further depletion and increase, respectively. Increased plasma free fatty acids (FAs) upon fasting suggested normal capacity for mobilization of lipids from white adipose tissue into circulation. Strikingly, however, serum glycerol concentration was not increased concomitantly with free FAs, suggesting its rapid uptake into the liver and utilization for fuel or gluconeogenesis in the mutants. The mutant hepatocyte mitochondria were capable of responding to fasting by appropriate morphological changes, as analyzed by electron microscopy, and by increasing respiration. Mutants showed increased hepatic gene expression of major metabolic controllers typically associated with fasting response (Ppargc1a, Fgf21, Cd36) already in the fed state, suggesting a chronic starvation-like metabolic condition. Despite this, the mutant mice responded largely normally to fasting by increasing hepatic respiration and switching to FA utilization, indicating that the mechanisms driving these adaptations are not compromised by the CIII dysfunction. SUMMARY STATEMENT Bcs1l mutant mice with severe CIII deficiency, energy deprivation and post-weaning lipolysis respond to fasting similarly to wild-type mice, suggesting largely normal systemic lipid mobilization and utilization mechanisms.

Asunto(s)

Complejo III de Transporte de Electrones/metabolismo; Ayuno/fisiología; Movilización Lipídica/fisiología; Acidosis Láctica/metabolismo; Animales; Glucemia/metabolismo; Colestasis/metabolismo; Transporte de Electrón/fisiología; Femenino; Retardo del Crecimiento Fetal/metabolismo; Gluconeogénesis/fisiología; Glucógeno/metabolismo; Hemosiderosis/metabolismo; Hepatocitos/metabolismo; Hepatocitos/fisiología; Homocigoto; Hipoglucemia/metabolismo; Hipoglucemia/fisiopatología; Hígado/metabolismo; Hígado/fisiología; Masculino; Errores Innatos del Metabolismo/metabolismo; Ratones; Ratones Endogámicos C57BL; Mitocondrias/metabolismo; Mitocondrias/fisiología; Enfermedades Mitocondriales/congénito; Enfermedades Mitocondriales/metabolismo; Aminoacidurias Renales/metabolismo; Triglicéridos/metabolismo

Palabras clave

BCS1L; Fasting; Lipid metabolism; Liver disease; Mitochondrial disorder; OXPHOS

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Texto completo: 1 Colección: 01-internacional Banco de datos: MEDLINE Asunto principal: Ayuno / Complejo III de Transporte de Electrones / Movilización Lipídica Límite: Animals Idioma: En Revista: Biochim Biophys Acta Mol Basis Dis Año: 2020 Tipo del documento: Article

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