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Gains of glycosylation comprise an unexpectedly large group of pathogenic mutations
Authors:Vogt Guillaume  Chapgier Ariane  Yang Kun  Chuzhanova Nadia  Feinberg Jacqueline  Fieschi Claire  Boisson-Dupuis Stéphanie  Alcais Alexandre  Filipe-Santos Orchidée  Bustamante Jacinta  de Beaucoudrey Ludovic  Al-Mohsen Ibrahim  Al-Hajjar Sami  Al-Ghonaium Abdulaziz  Adimi Parisa  Mirsaeidi Mehdi  Khalilzadeh Soheila  Rosenzweig Sergio  de la Calle Martin Oscar  Bauer Thomas R  Puck Jennifer M  Ochs Hans D  Furthner Dieter  Engelhorn Carolin  Belohradsky Bernd  Mansouri Davood  Holland Steven M  Schreiber Robert D  Abel Laurent  Cooper David N  Soudais Claire  Casanova Jean-Laurent
Institution:Laboratory of Human Genetics of Infectious Diseases, University of Paris René Descartes INSERM U550, Necker Medical School, 156 rue de Vaugirard, 75015 Paris, France.
Abstract:Mutations involving gains of glycosylation have been considered rare, and the pathogenic role of the new carbohydrate chains has never been formally established. We identified three children with mendelian susceptibility to mycobacterial disease who were homozygous with respect to a missense mutation in IFNGR2 creating a new N-glycosylation site in the IFNgammaR2 chain. The resulting additional carbohydrate moiety was both necessary and sufficient to abolish the cellular response to IFNgamma. We then searched the Human Gene Mutation Database for potential gain-of-N-glycosylation missense mutations; of 10,047 mutations in 577 genes encoding proteins trafficked through the secretory pathway, we identified 142 candidate mutations ( approximately 1.4%) in 77 genes ( approximately 13.3%). Six mutant proteins bore new N-linked carbohydrate moieties. Thus, an unexpectedly high proportion of mutations that cause human genetic disease might lead to the creation of new N-glycosylation sites. Their pathogenic effects may be a direct consequence of the addition of N-linked carbohydrate.
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