The positive inotropic effect of pyruvate involves an increase in myofilament calcium sensitivity.

Pyruvate is a metabolic fuel that is a potent inotropic agent. Despite its unique inotropic and antioxidant properties, the molecular mechanism of its inotropic mechanism is still largely unknown. To examine the inotropic effect of pyruvate in parallel with intracellular calcium handling under near...

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Main Authors: Carlos A A Torres, Kenneth D Varian, Cynthia H Canan, Jonathan P Davis, Paul M L Janssen
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3655183?pdf=render
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author Carlos A A Torres
Kenneth D Varian
Cynthia H Canan
Jonathan P Davis
Paul M L Janssen
author_facet Carlos A A Torres
Kenneth D Varian
Cynthia H Canan
Jonathan P Davis
Paul M L Janssen
author_sort Carlos A A Torres
collection DOAJ
description Pyruvate is a metabolic fuel that is a potent inotropic agent. Despite its unique inotropic and antioxidant properties, the molecular mechanism of its inotropic mechanism is still largely unknown. To examine the inotropic effect of pyruvate in parallel with intracellular calcium handling under near physiological conditions, we measured pH, myofilament calcium sensitivity, developed force, and calcium transients in ultra thin rabbit heart trabeculae at 37 °C loaded iontophoretically with the calcium indicator bis-fura-2. By contrasting conditions of control versus sarcoplasmic reticulum block (with either cyclopiazonic acid and ryanodine or with thapsigargin) we were able to characterize and isolate the effects of pyruvate on sarcoplasmic reticulum calcium handling and developed force. A potassium contracture technique was subsequently utilized to assess the force-calcium relationship and thus the myofilament calcium sensitivity. Pyruvate consistently increased developed force whether or not the sarcoplasmic reticulum was blocked (16.8±3.5 to 24.5±5.1 vs. 6.9±2.6 to 12.5±4.4 mN/mm(2), non-blocked vs. blocked sarcoplasmic reticulum respectively, p<0.001, n = 9). Furthermore, the sensitizing effect of pyruvate on the myofilaments was demonstrated by potassium contractures (EC50 at baseline versus 20 minutes of pyruvate infusion (peak force development) was 701±94 vs. 445±65 nM, p<0.01, n = 6). This study is the first to demonstrate that a leftward shift in myofilament calcium sensitivity is an important mediator of the inotropic effect of pyruvate. This finding can have important implications for future development of therapeutic strategies in the management of heart failure.
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spelling doaj.art-ec20097183f64ceaafb149f568075bf12022-12-22T01:51:57ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0185e6360810.1371/journal.pone.0063608The positive inotropic effect of pyruvate involves an increase in myofilament calcium sensitivity.Carlos A A TorresKenneth D VarianCynthia H CananJonathan P DavisPaul M L JanssenPyruvate is a metabolic fuel that is a potent inotropic agent. Despite its unique inotropic and antioxidant properties, the molecular mechanism of its inotropic mechanism is still largely unknown. To examine the inotropic effect of pyruvate in parallel with intracellular calcium handling under near physiological conditions, we measured pH, myofilament calcium sensitivity, developed force, and calcium transients in ultra thin rabbit heart trabeculae at 37 °C loaded iontophoretically with the calcium indicator bis-fura-2. By contrasting conditions of control versus sarcoplasmic reticulum block (with either cyclopiazonic acid and ryanodine or with thapsigargin) we were able to characterize and isolate the effects of pyruvate on sarcoplasmic reticulum calcium handling and developed force. A potassium contracture technique was subsequently utilized to assess the force-calcium relationship and thus the myofilament calcium sensitivity. Pyruvate consistently increased developed force whether or not the sarcoplasmic reticulum was blocked (16.8±3.5 to 24.5±5.1 vs. 6.9±2.6 to 12.5±4.4 mN/mm(2), non-blocked vs. blocked sarcoplasmic reticulum respectively, p<0.001, n = 9). Furthermore, the sensitizing effect of pyruvate on the myofilaments was demonstrated by potassium contractures (EC50 at baseline versus 20 minutes of pyruvate infusion (peak force development) was 701±94 vs. 445±65 nM, p<0.01, n = 6). This study is the first to demonstrate that a leftward shift in myofilament calcium sensitivity is an important mediator of the inotropic effect of pyruvate. This finding can have important implications for future development of therapeutic strategies in the management of heart failure.http://europepmc.org/articles/PMC3655183?pdf=render
spellingShingle Carlos A A Torres
Kenneth D Varian
Cynthia H Canan
Jonathan P Davis
Paul M L Janssen
The positive inotropic effect of pyruvate involves an increase in myofilament calcium sensitivity.
PLoS ONE
title The positive inotropic effect of pyruvate involves an increase in myofilament calcium sensitivity.
title_full The positive inotropic effect of pyruvate involves an increase in myofilament calcium sensitivity.
title_fullStr The positive inotropic effect of pyruvate involves an increase in myofilament calcium sensitivity.
title_full_unstemmed The positive inotropic effect of pyruvate involves an increase in myofilament calcium sensitivity.
title_short The positive inotropic effect of pyruvate involves an increase in myofilament calcium sensitivity.
title_sort positive inotropic effect of pyruvate involves an increase in myofilament calcium sensitivity
url http://europepmc.org/articles/PMC3655183?pdf=render
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