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| Indexado |
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| DOI | 10.1016/J.CBPB.2017.12.008 | ||||
| Año | 2018 | ||||
| Tipo | artículo de investigación |
Citas Totales
Autores Afiliación Chile
Instituciones Chile
% Participación
Internacional
Autores
Afiliación Extranjera
Instituciones
Extranjeras
Mammalian hibernation is characterized by extensive adjustments to metabolism that typically include suppression of carbohydrate catabolism and a switch to triglycerides as the primary fuel during torpor. A crucial locus of control in this process is the pyruvate dehydrogenase complex that gates carbohydrate entry into the tricarboxylic acid cycle. Within the complex, the El enzyme pyruvate dehydrogenase (PDH) is the main regulatory site and is subject to inhibitory phosphorylation at three serine residues (S232, S293, S300). To determine if marsupial hibernators show a comparable focus on PDH to regulate fuel metabolism, the current study explored PDH control by site-specific phosphorylation in the South American marsupial, monito del monte (Dromiciops gliroides). Luminex multiplex technology was used to analyze PDH responses in six tissues comparing control and hibernating (4 days continuous torpor) animals. Total PDH content did not change significantly during hibernation in any tissue but phospho-PDH content increased in all. Heart PDH showed increased phosphorylation at all three sites by 8.1-, 10.6- and 2.1-fold for S232, 5293 and S300, respectively. Liver also showed elevated p-S300 (2.5-fold) and p-S293 (4.7-fold) content. Phosphorylation of S232 and S293 increased significantly in brain and lung but only S232 phosphorylation increased in kidney and skeletal muscle. The results show that PDH suppression via enzyme phosphorylation during torpor is a conserved mechanism for inhibiting carbohydrate catabolism in both marsupial and eutherian mammals, an action that would also promote the switch to fatty acid oxidation instead.
| Revista | ISSN |
|---|---|
| Comparative Biochemistry And Physiology B Biochemistry & Molecular Biology | 1096-4959 |
| Ord. | Autor | Género | Institución - País |
|---|---|---|---|
| 1 | Wijenayake, Sanoji | - |
CARLETON UNIV - Canadá
Carleton University - Canadá |
| 2 | Luu, Bryan E. | Hombre |
CARLETON UNIV - Canadá
Carleton University - Canadá |
| 3 | Zhang, Jing | - |
CARLETON UNIV - Canadá
Western Univ - Canadá Carleton University - Canadá Western University - Canadá Schulich School of Medicine & Dentistry - Canadá |
| 4 | Tessier, Shannon N. | Mujer |
CARLETON UNIV - Canadá
MASSACHUSETTS GEN HOSP - Estados Unidos Harvard Med Sch - Estados Unidos Carleton University - Canadá Massachusetts General Hospital - Estados Unidos |
| 5 | Quintero-Galvis, Julian F. | Hombre |
Universidad Austral de Chile - Chile
|
| 6 | Gaitan-Espitia, Juan-Diego | Hombre |
CSIRO Oceans & Atmosphere - Australia
CSIRO Oceans and Atmosphere - Australia |
| 7 | NESPOLO-ROSSI, ROBERTO FERNANDO | Hombre |
Universidad Austral de Chile - Chile
|
| 8 | Storey, Kenneth B. | Hombre |
CARLETON UNIV - Canadá
Carleton University - Canadá |
| Fuente |
|---|
| Fondo Nacional de Desarrollo Científico y Tecnológico |
| Comisión Nacional de Investigación Científica y Tecnológica |
| Natural Sciences and Engineering Research Council of Canada |
| Fondo Nacional de Desarrollo Científico, Tecnológico y de Innovación Tecnológica |
| Heart and Stroke Foundation of Canada |
| Queen Elizabeth II Graduate Scholarship in Science and Technology |
| FONDECYT grant Chile |
| NSERC Postdoctoral Fellowship |
| Discovery grant from the Natural Sciences and Engineering Research Council (NSERC) Canada |
| NSERC Canada CGS-D |
| Conicyt doctoral fellowship, Chile |
| Canada Research Chair in Molecular Physiology |
| Agradecimiento |
|---|
| We thank J.M. Storey for editorial review of the manuscript. This work was supported by a grant-in-aid from the Heart and Stroke Foundation of Canada (#0005874) and a Discovery grant (#6793) from the Natural Sciences and Engineering Research Council (NSERC) Canada to K.B.S. and a FONDECYT grant Chile (#1130750) to R.F.N. Scholarship funding supported S.W. (Queen Elizabeth II Graduate Scholarship in Science and Technology), B.E.L. (NSERC Canada CGS-D), S.N.T. (NSERC Postdoctoral Fellowship), and J. Quintero-Galvis (Conicyt doctoral fellowship, Chile). K.B.S. holds the Canada Research Chair in Molecular Physiology. |
| We thank J.M. Storey for editorial review of the manuscript. This work was supported by a grant-in-aid from the Heart and Stroke Foundation of Canada (#0005874) and a Discovery grant (#6793) from the Natural Sciences and Engineering Research Council (NSERC) Canada to K.B.S. and a FONDECYT grant Chile (#1130750) to R.F.N. Scholarship funding supported S.W. (Queen Elizabeth II Graduate Scholarship in Science and Technology), B.E.L. (NSERC Canada CGS-D), S.N.T. (NSERC Postdoctoral Fellowship), and J. Quintero-Galvis (Conicyt doctoral fellowship, Chile). K.B.S. holds the Canada Research Chair in Molecular Physiology. |