The effects of dichloroacetate on lactate accumulation and endurance in an exercising rat model

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Deutscher übersetzter Titel:Auswirkungen von Dichloroacetat auf Laktatakkumulation und Ausdauer bei trainierenden Ratten im Tierversuch
Autor:Durkot, M.J.; De Garavilla, L.; Caretti, D.; Francesconi, R.
Erschienen in:International journal of sports medicine
Veröffentlicht:16 (1995), 3, S. 167-171, Lit.
Format: Literatur (SPOLIT)
Publikationstyp: Zeitschriftenartikel
Medienart: Gedruckte Ressource Elektronische Ressource (online)
Sprache:Englisch
ISSN:0172-4622, 1439-3964
DOI:10.1055/s-2007-972986
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Erfassungsnummer:PU199509102908
Quelle:BISp

Abstract des Autors

Severe lactic acidosis usually accompanies intense endurance exercise. It has been postulated that glycogen depletion working in concert with elevated muscle and plasma lactate levels lead to a concomitant reduction in pH. Their cumulative effect during prolonged physical exertion now leads to muscular fatigue and eventually limit endurance capacity. Therefore in the present study, dichloroacetate (DCA), a compound which enhances the rate or pyruvate oxidation thus reducing lactate formation, has been evaluated in a validated rat model of sub-maximal exercise performance. Male rats (350 g) were divided into two groups (control-saline, IV and DCA 5 mg/kg, IV) and were exercised to exhaustion in a chamber (26øC) on a treadmill (11 m/min, 6ø incline). When compared to controls, the DCA-treated rats had longer run times (169 vs 101 min) and a decreased heating rate (0.020 vs 0.029øC/min). In addition, DCA attenuated the increase in plasma lactate (28 vs 40 mg/dl) and significantly reduced both the rate and absolute amount of depletion of muscle glycogen stores. These results suggest that the activation of pyruvate dehydrogenase activity by DCA resulted in a reduction in the rate of glycogenolysis in addition to decreasing lactate accumulation by presumably limiting the availability of pyruvate for conversion to lactate, therefore increasing muscle carbohydrate oxidation via the TCA cycle. Thus DCA effected a significant delay in muscle fatigue. Verf.-Referat