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Tissue-specific cytochrome c oxidase assembly defects due to mutations in SCO2 and SURF1

Publication at First Faculty of Medicine |
2005

Abstract

The biogenesis of eukaryotic COX (cytochrome c oxidase) requires several accessory proteins in addition to structural subunits and prosthetic groups. We have analysed the assembly state of COX and SC02 protein levels in various tissues of six patients with mutations in SC02 and SURF1.

SC02 is a copper-binding protein presumably involved in formation of the Cu-A centre of the COX2 subunit. The function of SURF1 is unknown.

Immunoblot analysis of native gels demonstrated that COX holoenzyme is reduced to 10-20% in skeletal muscle and brain of SC02 and SURF1 patients and to 10-30% in heart of SC02 patients, whereas liver of SC02 patients' contained normal holoenzyme levels. The steady-state levels of mutant SC02 protein ranged from 0 to 20% in different SC02 patient tissues.

In addition, eight distinct COX subcomplexes and unassembled subunits were found, some of them identical with known assembly intermediates of the human enzyme. Heart, brain and skeletal muscle of SC02 patients contained accumulated levels of the COX1(.)COX4(.) COX5A subcomplex, three COX1-containing subcomplexes, a COX4(.)COX5A subcomplex and two subcomplexes composed of only COX4 or COX5A.

The accumulation of COX 1(.)COX4(.) COX5A subcomplex, along with the virtual absence of free COX2, suggests that the lack of the Cu-A centre may result in decreased stability of COX2. The appearance of COX4(.)COX5A subcomplex indicates that association of these nucleus-encoded subunits probably precedes their addition to COX1 during the assembly process.

Finally, the consequences of SC02 and SURF1 mutations suggest the existence of tissue-specific functional differences of these proteins that may serve different tissue-specific requirements for the regulation of COX biogenesis.