[No authors listed]
BACKGROUND:Necdin, a MAGE family protein expressed primarily in the nervous system, has been shown to interact with both nuclear and cytoplasmic proteins, but the mechanism of its nucleocytoplasmic transport are unknown. METHODOLOGY/PRINCIPAL FINDINGS:We carried out a large-scale interaction screen using necdin as a bait in the yeast RRS system, and found a wide range of potential interactors with different subcellular localizations, including over 60 new candidates for direct binding to necdin. Integration of these interactions into a comprehensive network revealed a number of coherent interaction modules, including a cytoplasmic module connecting to necdin through huntingtin-associated protein 1 (Hap1), dynactin and hip-1 protein interactor (Hippi); a nuclear P53 and Creb-binding-protein (Crebbp) module, connecting through Crebbp and WW domain-containing transcription regulator protein 1 (Wwtr1); and a nucleocytoplasmic transport module, connecting through transportins 1 and 2. We validated the necdin-transportin1 interaction and characterized a sequence motif in necdin that modulates karyopherin interaction. Surprisingly, a D234P necdin mutant showed enhanced binding to both transportin1 and importin β1. Finally, exclusion of necdin from the nucleus triggered extensive cell death. CONCLUSIONS/SIGNIFICANCE:These data suggest that necdin has multiple roles within protein complexes in different subcellular compartments, and indicate that it can utilize multiple karyopherin-dependent pathways to modulate its localization.
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Tyw1, Tada3, Rcbtb2, Otub1, Thoc5, Sobp, Cacybp, Cdh2, Cdh4, Cdh5, Ctbp2, Dctn1, Hap1, Hcfc1, Itgb5, Kif21b, Lamb1, Ndn, Nefl, Nin, Nucb1, Pex19, Rpl28, Med22, Iffo2, Tbrg1, Ncaph, Ccm2, Tuba1a, Uqcrc1, Dner, Pogz, Dazap2, Angptl2, Ncoa4, Ddx24, Cabp1, Iffo1, Copb2, Camk1, Tdp2, Eid1, Huwe1, 2610301B20Rik, Mpnd, Mcm10, Mier2, Rufy2, Tbc1d9, Ttc4, Pcdh18, Dcbld2, Ift57, Nfx1, Chmp4b, Ppfia3, Chmp5, Rnf114, Wwtr1, Strn4, Myl9, Ndn, Tnpo1, KPNB1, TNPO1, NDN
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