Functional study in a yeast model of a novel succinate dehydrogenase subunit B gene germline missense mutation (C191Y) diagnosed in a patient affected by a glomus tumor

doi:10.1093/hmg/ddp102

Human Molecular Genetics Advance Access originally published online on March 4, 2009
Human Molecular Genetics 2009 18(10):1860-1868; doi:10.1093/hmg/ddp102

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Functional study in a yeast model of a novel succinate dehydrogenase subunit B gene germline missense mutation (C191Y) diagnosed in a patient affected by a glomus tumor

Paola Goffrini¹^,, Tonino Ercolino²^,, Elena Panizza¹, Valentino Giachè², Leonardo Cavone³, Alberto Chiarugi³, Veronica Dima¹, Iliana Ferrero¹^,* and Massimo Mannelli²

¹ Department of Genetics, Biology of Microorganisms, Anthropology and Evolution, University of Parma, Viale Usberti 11/A, 43100 Parma, Italy ² Section of Endocrinology, Department of Clinical Pathophysiology, University of Florence Medical School, 50139 Florence, Italy ³ Department of Preclinical and Clinical Pharmacology, University of Florence, 50139 Florence, Italy

^* To whom correspondence should be addressed. Tel: +39 0521905600; Fax: +39 0521905604; Email: iferrero{at}unipr.it

Received January 30, 2009; Accepted March 2, 2009

Mutations of succinate dehydrogenase (SDH) subunits B, C andD are associated to pheochromocytoma/paraganglioma (PGL) development.The mechanisms linking SDH mutations to tumorigenesis are currentlyunknown. We report a novel germline missense SDHB mutation (C191Y)in a patient affected by a glomus tumor. The missense mutationhits an amino acid residue conserved from mammals to the yeastSaccharomyces cerevisiae. The pathogenic significance of thehuman mutation was validated in a yeast model. SDH2^C184Y mutantallele equivalent to human SDHB^C191Y did not restore the OXPHOSphenotype of the ${Delta}$ sdh2 null mutant. In the mutant, SDH activitywas also abolished along with a reduction in respiration. Sensitivityto oxidative stress was increased in the mutant, as revealedby reduced growth in the presence of menadione. Remarkably,the frequency of petite colony formation was increased in themutant yeast strain, indicating an increased mtDNA mutability.Histochemistry demonstrates that SDH activity was selectivelyabsent in the patient tumor tissue. Overall, our results demonstratethat the C191Y SDHB mutation suppresses SDH enzyme activityleading to increased ROS formation and mtDNA mutability in ouryeast model. These findings further our understanding of themechanisms underlying PGL development and point to the yeastmodel as a valid tool to investigate on the possible pathogenicrelevance of SDH novel mutations and/or rare polymorphism.

The authors wish to be known that, in their opinion, the firsttwo authors should be regarded as joint First Authors.

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