AIRE-PHD fingers are structural hubs to maintain the integrity of chromatin-associated interactome

نویسندگان

  • Massimiliano Gaetani
  • Vittoria Matafora
  • Mario Saare
  • Dimitrios Spiliotopoulos
  • Luca Mollica
  • Giacomo Quilici
  • Francesca Chignola
  • Valeria Mannella
  • Chiara Zucchelli
  • Pärt Peterson
  • Angela Bachi
  • Giovanna Musco
چکیده

Mutations in autoimmune regulator (AIRE) gene cause autoimmune polyendocrinopathy candidiasis ectodermal dystrophy. AIRE is expressed in thymic medullary epithelial cells, where it promotes the expression of peripheral-tissue antigens to mediate deletional tolerance, thereby preventing self-reactivity. AIRE contains two plant homeodomains (PHDs) which are sites of pathological mutations. AIRE-PHD fingers are important for AIRE transcriptional activity and presumably play a crucial role in the formation of multimeric protein complexes at chromatin level which ultimately control immunological tolerance. As a step forward the understanding of AIRE-PHD fingers in normal and pathological conditions, we investigated their structure and used a proteomic SILAC approach to assess the impact of patient mutations targeting AIRE-PHD fingers. Importantly, both AIRE-PHD fingers are structurally independent and mutually non-interacting domains. In contrast to D297A and V301M on AIRE-PHD1, the C446G mutation on AIRE-PHD2 destroys the structural fold, thus causing aberrant AIRE localization and reduction of AIRE target genes activation. Moreover, mutations targeting AIRE-PHD1 affect the formation of a multimeric protein complex at chromatin level. Overall our results reveal the importance of AIRE-PHD domains in the interaction with chromatin-associated nuclear partners and gene regulation confirming the role of PHD fingers as versatile protein interaction hubs for multiple binding events.

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عنوان ژورنال:

دوره 40  شماره 

صفحات  -

تاریخ انتشار 2012