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Network Analysis of UBE3A/E6AP-Associated Proteins Provides Connections to Several Distinct Cellular Processes
Authors:Gustavo Martínez-Noël  Katja Luck  Simone Kühnle  Alice Desbuleux  Patricia Szajner  Jeffrey T. Galligan  Diana Rodriguez  Leon Zheng  Kathleen Boyland  Flavian Leclere  Quan Zhong  David E. Hill  Marc Vidal  Peter M. Howley
Affiliation:1. Department of Microbiology and Immunobiology, Harvard Medical School, Boston, MA 02115, USA;2. Center for Cancer Systems Biology (CCSB), Dana-Farber Cancer Institute, Boston, MA 02115, USA;3. Department of Genetics, Harvard Medical School, Boston, MA 02115, USA;4. Department of Cancer Biology, Dana-Farber Cancer Institute, Boston, MA 02115, USA;5. GIGA-R, University of Liège, Liège 4000, Belgium
Abstract:Perturbations in activity and dosage of the UBE3A ubiquitin-ligase have been linked to Angelman syndrome and autism spectrum disorders. UBE3A was initially identified as the cellular protein hijacked by the human papillomavirus E6 protein to mediate the ubiquitylation of p53, a function critical to the oncogenic potential of these viruses. Although a number of substrates have been identified, the normal cellular functions and pathways affected by UBE3A are largely unknown. Previously, we showed that UBE3A associates with HERC2, NEURL4, and MAPK6/ERK3 in a high-molecular-weight complex of unknown function that we refer to as the HUN complex (HERC2, UBE3A, and NEURL4). In this study, the combination of two complementary proteomic approaches with a rigorous network analysis revealed cellular functions and pathways in which UBE3A and the HUN complex are involved. In addition to finding new UBE3A-associated proteins, such as MCM6, SUGT1, EIF3C, and ASPP2, network analysis revealed that UBE3A-associated proteins are connected to several fundamental cellular processes including translation, DNA replication, intracellular trafficking, and centrosome regulation. Our analysis suggests that UBE3A could be involved in the control and/or integration of these cellular processes, in some cases as a component of the HUN complex, and also provides evidence for crosstalk between the HUN complex and CAMKII interaction networks. This study contributes to a deeper understanding of the cellular functions of UBE3A and its potential role in pathways that may be affected in Angelman syndrome, UBE3A-associated autism spectrum disorders, and human papillomavirus-associated cancers.
Keywords:AP-MS  affinity purifications followed by identification of proteins by liquid chromatography-tandem mass spectrometry  AS  Angelman syndrome  ASD  autism spectrum disorders  CompPASS  Comparative Proteomic Analysis Software Suite  HCIPs  high-confidence interacting proteins  HPV  human papillomavirus  HPV16  human papillomavirus type 16  hrHPVs  high-risk human papillomavirus  HUN complex  protein complex containing HERC2, UBE3A, and NEURL4  Y2H  yeast two hybrid  Y3H  yeast three hybrid.  Angelman syndrome  autism  human papillomavirus  cervical cancer  proteomics
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