Effects of metformin and other biguanides on oxidative phosphorylation in mitochondria
We report that biguanides inhibit complex I by inhibiting ubiquinone reduction (but not competitively) and, independently, stimulate reactive oxygen species production by the complex I flavin. Biguanides also inhibit mitochondrial ATP synthase, and two of them inhibit only ATP hydrolysis, not synthesis. Thus, we identify biguanides as a new class of complex I and ATP synthase inhibitor. By comparing biguanide effects on isolated complex I and cultured cells, we distinguish three anti-diabetic and potentially anti-neoplastic biguanides (metformin, buformin and phenformin) from two anti-malarial biguanides (cycloguanil and proguanil): the former are accumulated into mammalian mitochondria and affect oxidative phosphorylation, whereas the latter are excluded so act only on the parasite. Our mechanistic and pharmacokinetic insights are relevant to understanding and developing the role of biguanides in new and existing therapeutic applications, including cancer, diabetes, and malaria.
Source: BJ Energy - Category: Biochemistry Authors: H R Bridges, A J Y Jones, M N Pollak, J Hirst Tags: BJ Energy Source Type: research
More News: Biochemistry | Cancer | Cancer & Oncology | Diabetes | Endocrinology | Fortamet | Laboratory Medicine | Malaria | Metformin | Mitochondria | Parasitic Diseases | Parasitology | Respiratory Medicine
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