Mechanism of the antimycin A-mediated enhancement oft-butylhydroperoxide-induced single-strand breakage in DNA

Author:

GUIDARELLI Andrea1,CLEMENTI Emilio2,BRAMBILLA Liliana1,CANTONI Orazio1

Affiliation:

1. Istituto di Farmacologia e Farmacognosia and Centro di Farmacologia Oncologica Sperimentale, Università di Urbino, Via S. Chiara, 27, 61029 Urbino (PS), Italy

2. Dipartimento di Farmacologia, Università di Reggio Calabria, 88021 Roccelletta di Borgia, Catanzaro and Consiglio Nazionale delle Ricerche, Molecular and Cellular Pharmacology Centre, DIBIT-San Raffaele Scientific Institute, Via Olgettina 58, 20132 Milano, Italy

Abstract

Inhibitors of complex III increased the DNA strand scission induced by t-butylhydroperoxide (tB-OOH) and cumene hydroperoxide but did not affect DNA damage induced by H2O2. The hypothesis that these effects are selectively linked to inhibition of the electron transport from cytochrome b to cytochrome c1 is validated by the following observations: (1) two complex III inhibitors, antimycin A and 2-heptyl-4-hydroxyquinoline N-oxide, enhanced the tB-OOH-induced DNA cleavage over the same concentration range as that in which inhibition of oxygen consumption was observed; (2) the complex III inhibitor-mediated enhancement of tB-OOH-induced DNA damage was abolished by the complex I inhibitor rotenone or by glucose omission, and (3) the enhancing effects of antimycin A were not observed in respiration-deficient cells. The mechanism whereby the complex III inhibitors potentiate DNA cleavage promoted by tB-OOH was subsequently investigated with intact as well as permeabilized cells. H2O2, produced at the level of mitochondria via a Ca2+-dependent process, was found to account for the enhancing effects of antimycin A.

Publisher

Portland Press Ltd.

Subject

Cell Biology,Molecular Biology,Biochemistry

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