Human SCO2 is required for the synthesis of CO II and as a thiol-disulphide oxidoreductase for SCO1

doi:10.1093/hmg/ddp158

Human Molecular Genetics Advance Access originally published online on March 31, 2009
Human Molecular Genetics 2009 18(12):2230-2240; doi:10.1093/hmg/ddp158

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Human SCO2 is required for the synthesis of CO II and as a thiol-disulphide oxidoreductase for SCO1

Scot C. Leary¹^,, Florin Sasarman¹^,, Tamiko Nishimura¹ and Eric A. Shoubridge¹^,2^,*

¹ Montreal Neurological Institute, McGill University, 3801 University Street, Montreal, Quebec, Canada H3A 2B4 ² Department of Human Genetics, McGill University, Montreal, Canada H3A 2B4

^* To whom correspondence should be addressed. Tel: +1 5143988523; Fax: +1 5143981509; Email: eric{at}ericpc.mni.mcgill.ca

Received February 6, 2009; Accepted March 25, 2009

Human SCO1 and SCO2 code for essential metallochaperones withill-defined functions in the biogenesis of the Cu_A site of cytochromec oxidase subunit II (CO II). Here, we have used patient celllines to investigate the specific roles of each SCO proteinin this pathway. By pulse-labeling mitochondrial translationproducts, we demonstrate that the synthesis of CO II is reducedin SCO2, but not in SCO1, cells. Despite this biosynthetic defect,newly synthesized CO II is more stable in SCO2 cells than incontrol cells. RNA_i-mediated knockdown of mutant SCO2 abolishesCO II labeling in the translation assay, whereas knockdown ofmutant SCO1 does not affect CO II synthesis. These results indicatethat SCO2 acts upstream of SCO1, and that it is indispensablefor CO II synthesis. The subsequent maturation of CO II is contingentupon the formation of a complex that includes both SCO proteins,each with a functional CxxxC copper-coordinating motif. In controlcells, the cysteines in this motif in SCO1 exist as a mixedpopulation comprised of oxidized disulphides and reduced thiols;however, the relative ratio of oxidized to reduced cysteinesin SCO1 is perturbed in cells from both SCO backgrounds. Overexpressionof wild-type SCO2, or knockdown of mutant SCO2, in SCO2 cellsalters the ratio of oxidized to reduced cysteines in SCO1, suggestingthat SCO2 acts as a thiol-disulphide oxidoreductase to oxidizethe copper-coordinating cysteines in SCO1 during CO II maturation.Based on these data we present a model in which each SCO proteinfulfills distinct, stage-specific functions during CO II synthesisand Cu_A site maturation.

The authors wish it to be known that, in their opinion, thefirst two authors should be regarded as joint First Authors.

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