Different proteomic strategies to identify genuine SUMO targets and their modification sites in Trypanosoma brucei procyclic forms

cic.isFulltexttruees
cic.isPeerReviewedtruees
cic.lugarDesarrolloInstituto de Investigaciones Biotecnológicas - Instituto Tecnológico Chascomús es
cic.versioninfo:eu-repo/semantics/publishedVersionen
dc.date.accessioned2018-05-15T17:58:02Z
dc.date.available2018-05-15T17:58:02Z
dc.identifier.urihttps://digital.cic.gba.gob.ar/handle/11746/7295
dc.titleDifferent proteomic strategies to identify genuine SUMO targets and their modification sites in Trypanosoma brucei procyclic formsen
dc.typeArtículoes
dcterms.abstractSUMOylation is an important post-translational modification conserved in eukaryotic organisms. In Trypanosoma brucei, SUMO (Small Ubiquitinlike MOdifier) is essential in procyclic and bloodstream forms. Furthermore, SUMO has been linked to the antigenic variation process, as a highly SUMOylated focus was recently identified within chromatin-associated proteins of the active variant surface glycoprotein expression site. We aimed to establish a reliable strategy to identify SUMO conjugates in T. brucei. We expressed various tagged variants of SUMO from the endogenous locus. HisHA-TbSUMO was useful to validate the tag functionality but SUMO conjugates were not enriched enough over contaminants after affinity purification. A Lys-deficient SUMO version, created to reduce contaminants by Lys-C digestion, was able to overcome this issue but did not allow mapping many SUMOylation sites. This cell line was in turn useful to demonstrate that polySUMO chains are not essential for parasite viability. Finally, a HisHA-TbSUMOT106K version allowed the purification of SUMO conjugates and, after digestion with Lys-C, the enrichment for diGly-Lys peptides using specific antibodies. This site-specific proteomic strategy led us to identify 45 SUMOylated proteins and 53 acceptor sites unambiguously. SUMOylated proteins belong mainly to nuclear processes, such as DNA replication and repair, transcription, rRNA biogenesis and chromatin remodelling, among others.en
dcterms.creator.authorIribarren, Paula Anaes
dcterms.creator.authorBerazategui, María Agustinaes
dcterms.creator.authorBayona, Julio Cesares
dcterms.creator.authorAlmeida, Igores
dcterms.creator.authorCazzulo, Juan Josées
dcterms.creator.authorÁlvarez, Vanina Ederes
dcterms.extent10 p.es
dcterms.identifier.otherdoi:10.1111/cmi.12467es
dcterms.identifier.urlRecurso onlinees
dcterms.isPartOf.issuevol. 17, no. 10es
dcterms.isPartOf.seriesCellular Microbiologyes
dcterms.issued2015-10
dcterms.languageIngléses
dcterms.licenseAttribution-NonCommercial-NoDerivatives 4.0 International (BY-NC-ND 4.0)*
dcterms.subjecttrypanosomaen
dcterms.subjectSUMOes
dcterms.subjectproteomices
dcterms.subject.materiaCiencias Biológicases

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