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Role of microtubules in the regulation of metabolism in isolated cerebral microvessels
Department of Physiology, University of Missouri-Columbia, Columbia, Missouri 65212 We used 13 C-labeled substrates and nuclear magnetic resonance spectroscopy to examine carbohydrate metabolism in vascular smooth muscle of freshly isolated pig cerebral microvessels (PCMV). PCMV utilized [2- 13 C]gl...
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| Published in: | American Journal of Physiology: Cell Physiology 1999-12, Vol.277 (6), p.C1250-C1262 |
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| Main Authors: | , |
| Format: | Article |
| Language: | English |
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| Online Access: | Get full text |
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| Summary: | Department of Physiology, University of Missouri-Columbia, Columbia,
Missouri 65212
We used
13 C-labeled substrates and nuclear
magnetic resonance spectroscopy to examine carbohydrate metabolism in
vascular smooth muscle of freshly isolated pig cerebral microvessels
(PCMV). PCMV utilized
[2- 13 C]glucose mainly
for glycolysis, producing
[2- 13 C]lactate.
Simultaneously, PCMV utilized the glycolytic intermediate [1- 13 C]fructose
1,6-bisphosphate (FBP) mainly for gluconeogenesis, producing
[1- 13 C]glucose with
only minor
[3- 13 C]lactate
production. The dissimilarity in metabolism of
[2- 13 C]FBP derived
from [2- 13 C]glucose
breakdown and metabolism of exogenous
[1- 13 C]FBP
demonstrates that carbohydrate metabolism is compartmented in PCMV.
Because glycolytic enzymes interact with microtubules, we disrupted
microtubules with vinblastine. Vinblastine treatment significantly
decreased
[2- 13 C]lactate peak
intensity (87.8 ± 3.7% of control). The microtubule-stabilizing agent taxol also reduced
[2- 13 C]lactate peak
intensity (90.0 ± 2.4% of control). Treatment with both agents
further decreased
[2- 13 C]lactate
production (73.3 ± 4.0% of control). Neither vinblastine, taxol,
or the combined drugs affected
[1- 13 C]glucose peak
intensity (gluconeogenesis) or disrupted the compartmentation of
carbohydrate metabolism. The similar effects of taxol and vinblastine, drugs that have opposite effects on microtubule assembly, suggest that
they produce their effects on glycolytic rate by competing with
glycolytic enzymes for binding, not by affecting the overall assembly
state of the microtubule network. Glycolysis, but not gluconeogenesis,
may be regulated in part by glycolytic enzyme-microtubule interactions.
vascular smooth muscle; carbohydrate metabolism; tubulin; glycolytic enzymes; carbon-13 nuclear magnetic resonance; taxol; vinblastine; cytoarchitecture; gluconeogenesis |
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| ISSN: | 0363-6143 1522-1563 |
| DOI: | 10.1152/ajpcell.1999.277.6.c1250 |