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Quantitative proteomics reveals neuronal ubiquitination of Rngo/Ddi1 and several proteasomal subunits by Ube3a, accounting for the complexity of Angelman …

Human Molecular Genetics. 2018; 
Juanma Ramirez, Benoit Lectez, Nerea Osinalde, Monika Sivá, Nagore Elu, Kerman Aloria, Michaela Procházková, Coralia Perez, Jose Martínez-Hernández, Rosa Barrio, Klára Grantz Šašková, Jesus M Arizmendi, Ugo Mayor
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Gene Synthesis  Gene for human DDI1 protein (Uniprot Q8WTU0) was synthesized by GenScript and further amplified using the DDI1-Fw (5′-TATAGGTACCATGCTGATCACCGTG-3′) and DDI1-Rv (5′-TATAACCGGTATGCTCTTTTCGTCC-3′) primers and inserted between the Acc65I and AgeIsites of the DDI2-pEGFP-N1 vector, after the DDI2 gene had been removed using the same restriction enzymes. Get A Quote

摘要

Angelman syndrome is a complex neurodevelopmental disorder caused by the lack of function in the brain of a single gene, UBE3A. The E3 ligase coded by this gene is known to build K48-linked ubiquitin chains, a modification historically considered to target substrates for degradation by the proteasome. However, a change in protein abundance is not proof that a candidate UBE3A substrate is indeed ubiquitinated by UBE3A. We have here used an unbiased ubiquitin proteomics approach, the bioUb strategy, to identify 79 proteins that appear more ubiquitinated in the Drosophila photoreceptor cells when Ube3a is over-expressed. We found a significantly high number of those proteins to be proteasomal subunits or prote... More

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