Membrane fluidity changes are associated with benzo[a]pyrene-induced apoptosis in F258 cells: protection by exogenous cholesterol.

Polycyclic aromatic hydrocarbons (PAHs) such as benzo[a]yrene (B[a]P) constitute a widely distributed class of environmental pollutants, responsible for highly toxic effects. Elucidating the intracellular mechanisms of this cytotoxicity thus remains a major challenge. Besides the activation of the p53 apoptotic pathway, we have previously found in F258 hepatic cells that the B[a]P (50 nM)-induced apoptosis was also dependent upon the transmembrane transporter NHE1, whose activation might result from membrane alterations in our model. We here demonstrate that: (1) B[a]P induces a membrane fluidization surprisingly linked to NHE1 activation; (2) membrane stabilization by exogenous cholesterol protects cells from B[a]P-induced apoptosis, via an effect on late acidification and iron uptake.

Mots clés

benzo[a]pyrene apoptosis membrane fluidity NHE1 cholesterol

Domaines

Biologie cellulaire

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https://hal.science/hal-00699948

Soumis le : mardi 22 mai 2012-08:59:27

Dernière modification le : mardi 5 septembre 2023-11:22:04

Dates et versions

hal-00699948 , version 1 (22-05-2012)

Identifiants

HAL Id : hal-00699948 , version 1
DOI : 10.1196/annals.1378.011
PRODINRA : 405494
PUBMED : 17384252

Citer

Morgane Gorria, Xavier Tekpli, Odile Sergent, Laurence Huc, François Gaboriau, et al.. Membrane fluidity changes are associated with benzo[a]pyrene-induced apoptosis in F258 cells: protection by exogenous cholesterol.. Annals of the New York Academy of Sciences, 2006, 1090, pp.108-12. ⟨10.1196/annals.1378.011⟩. ⟨hal-00699948⟩

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