Cytochrome autocatalyzed carbonylation in the presence of hydrogen peroxide and cardiolipins.

Cytochrome (cyt ) is a small hemoprotein involved in electron shuttling in the mitochondrial respiratory chain and is now also recognized as an important mediator of apoptotic cell death. Its role in inducing programmed cell death is closely associated with the formation of a complex with the mitochondrion-specific phospholipid cardiolipin (CL), leading to a gain of peroxidase activity. However, the molecular mechanisms behind this gain and eventual cyt autoinactivation via its release from mitochondrial membranes remain largely unknown. Here, we examined the kinetics of the HO-mediated peroxidase activity of cyt both in the presence and absence of tetraoleoyl cardiolipin (TOCL)- and tetralinoleoyl cardiolipin (TLCL)-containing liposomes to evaluate the role of cyt -CL complex formation in the induction and stimulation of cyt peroxidase activity. Moreover, we examined peroxide-mediated cyt heme degradation to gain insights into the mechanisms by which cyt self-limits its peroxidase activity. Bottom-up proteomics revealed >50 oxidative modifications on cyt upon peroxide reduction. Of note, one of these by-products was the Tyr-based "cofactor" trihydroxyphenylalanine quinone (TPQ) capable of inducing deamination of Lys ϵ-amino groups and formation of the carbonylated product aminoadipic semialdehyde. In view of these results, we propose that autoinduced carbonylation, and thus removal of a positive charge in Lys, abrogates binding of cyt to negatively charged CL. The proposed mechanism may be responsible for release of cyt from mitochondrial membranes and ensuing inactivation of its peroxidase activity.