Cookies help us deliver our services. By using our services, you agree to our use of cookies. More information

Piel 2014 Acta Physiol (Oxf)

From Bioblast
Revision as of 16:24, 11 February 2015 by Bader Helga (talk | contribs)
Publications in the MiPMap
Piel S, Ehinger JK, Elmรฉr E, Hansson MJ (2014) Metformin induces lactate production in peripheral blood mononuclear cells and platelets through specific mitochondrial complex I inhibition. Acta Physiol (Oxf) [Epub ahead of print].

ยป PMID: 24801139

Piel S, Ehinger JK, Elmer E, Hansson MJ (2014) Acta Physiol (Oxf)

Abstract: AIM: Metformin is a widely used antidiabetic drug associated with the rare side effect of lactic acidosis which has been proposed to be linked to drug-induced mitochondrial dysfunction. Using respirometry, the aim of this study was to evaluate mitochondrial toxicity of metformin to human blood cells in relation to that of phenformin, a biguanide analogue withdrawn in most countries due to a high incidence of lactic acidosis.

METHODS: Peripheral blood mononuclear cells and platelets were isolated from healthy volunteers, and integrated mitochondrial function was studied in permeabilized and intact cells using high-resolution respirometry. A wide concentration range of metformin (0.1-100 mm) and phenformin (25-500 ฮผm) was investigated for dose- and time-dependent effects on respiratory capacities, lactate production and pH.

RESULTS: Metformin induced respiratory inhibition at complex I in peripheral blood mononuclear cells and platelets (IC50 0.45 mm and 1.2 mm respectively). Phenformin was about 20-fold more potent in complex I inhibition of platelets than metformin. Metformin further demonstrated a dose- and time-dependent respiratory inhibition and augmented lactate release at a concentration of 1 mm and higher.

CONCLUSION: Respirometry of human peripheral blood cells readily detected respiratory inhibition by metformin and phenformin specific to complex I, providing a suitable model for probing drug toxicity. Lactate production was increased at concentrations relevant for clinical metformin intoxication, indicating mitochondrial inhibition as a direct causative pathophysiological mechanism. Relative to clinical dosing, phenformin displayed a more potent respiratory inhibition than metformin, possibly explaining the higher incidence of lactic acidosis in phenformin-treated patients. โ€ข Keywords: Human, Drug screening, Metformin, Mitochondrial toxicity, Phenformin, Respirometry

โ€ข O2k-Network Lab: SE Lund Elmer E


Labels: MiParea: Respiration  Pathology: Diabetes 

Organism: Human  Tissue;cell: Blood cells  Preparation: Intact cells, Permeabilized cells 


Coupling state: LEAK, ROUTINE, OXPHOS, ETS"ETS" is not in the list (LEAK, ROUTINE, OXPHOS, ET) of allowed values for the "Coupling states" property. 

HRR: Oxygraph-2k 


Retrieved from "https://wiki.oroboros.at/index.php?title=Piel_2014_Acta_Physiol_(Oxf)&oldid=79878"
Powered by MediaWiki
Powered by Semantic MediaWiki