Publication | Open Access
Constitutive Expression of Bcl-3 in Thymocytes Increases the DNA Binding of NF-κB1 (p50) Homodimers In Vivo
99
Citations
57
References
1996
Year
Lymphocyte DevelopmentImmune RegulationImmunologyCell DeathImmunologic MechanismImmune SystemSignaling PathwayCell RegulationConstitutive ExpressionReceptor Tyrosine KinaseP50 HomodimersCell SignalingImmune SurveillanceCell BiologySignal TransductionDna BindingImmune Cell DevelopmentP52 HomodimersAnkyrin RepeatsTumor SuppressorCellular Immune ResponseMedicineCell Development
Previous studies have indicated that Bcl-3 interacts through its ankyrin repeats with the transcriptional factors NF-kappaB1 (p50) and NF-kappaB2 (p52), affecting their biological activities. To further investigate the role of Bcl-3 in vivo and its association with the NF-kappaB proteins, we have generated transgenic mice constitutively expressing Bcl-3 in thymocytes. The results indicate that Bcl-3 is associated with endogenous p50 and p52 in nuclear extracts from transgenic animals. Remarkably, constitutive expression of Bcl-3 in these cells augments the DNA binding activity of p52 homodimers. This effect could be reproduced in vitro and is blocked by anti-Bcl-3 antibodies. We have also shown that Bcl-3 is phosphorylated in thymocytes and that its dephosphorylation greatly decreases the effect on p50 homodimers.
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